CENTER FOR DRUG EVALUATION AND RESEARCH APPLICATION NUMBER: 2057180rig15000 OTHER PMR/PMC Development Template This template should be completed by the PMR/PMC Development Coordinator and included for each PMR/PMC in the Action Package. NDA # Product Name: 205,718 Akynzeo PMR/PMC Description: An 8-week GLP toxicology study with fertility evaluation in neonatal rats treated with netupitant alone. PMR/PMC Schedule Milestones: Final Protocol Submission: Study/Trial Completion: Final Report Submission: 05/30/2015 12/30/2015 03/30/2016 1. During application review, explain why this issue is appropriate for a PMR/PMC instead of a pre-approval requirement. Check type below and describe. Unmet need Life-threatening condition Long-term data needed Only feasible to conduct post-approval Prior clinical experience indicates safety Small subpopulation affected Theoretical concern Other A juvenile animal toxicity study with netupitant alone is needed to assure safety in a postmarketing pediatric trial of netupitant + palonosetron fixed dose combination to evaluate safety and efficacy. Dosing in the juvenile animal study should begin at a developmental stage comparable to the human neonatal stage. Based on results of the combination toxicity studies of netupitant + palonosetron in adult rats and dogs, and the toxicity profile of palonosetron alone in neonatal rats, juvenile animal studies with the drug combination are not considered necessary to support the pediatric study. 2. Describe the particular review issue and the goal of the study/clinical trial. If the study/clinical trial is a FDAAA PMR, describe the risk. If the FDAAA PMR is created post-approval, describe the “new safety information.” An oral toxicity study with netupitant alone of at least 8 weeks duration in neonatal rats is needed to support the enrollment of patients age 0 to < 12 years in the proposed pediatric clinical efficacy and safety study in patients age 0 to < 17 years. The neonatal rat study should include evaluation of developmental parameters, neurobehavioral effects, and fertility. PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 1 of 3 3. If the study/clinical trial is a PMR, check the applicable regulation. If not a PMR, skip to 4. - Which regulation? Accelerated Approval (subpart H/E) Animal Efficacy Rule Pediatric Research Equity Act FDAAA required safety study/clinical trial - If the PMR is a FDAAA safety study/clinical trial, does it: (check all that apply) Assess a known serious risk related to the use of the drug? Assess signals of serious risk related to the use of the drug? Identify an unexpected serious risk when available data indicate the potential for a serious risk? - If the PMR is a FDAAA safety study/clinical trial, will it be conducted as: Analysis of spontaneous postmarketing adverse events? Do not select the above study/clinical trial type if: such an analysis will not be sufficient to assess or identify a serious risk Analysis using pharmacovigilance system? Do not select the above study/clinical trial type if: the new pharmacovigilance system that the FDA is required to establish under section 505(k)(3) has not yet been established and is thus not sufficient to assess this known serious risk, or has been established but is nevertheless not sufficient to assess or identify a serious risk Study: all other investigations, such as investigations in humans that are not clinical trials as defined below (e.g., observational epidemiologic studies), animal studies, and laboratory experiments? Do not select the above study type if: a study will not be sufficient to identify or assess a serious risk Clinical trial: any prospective investigation in which the sponsor or investigator determines the method of assigning investigational product or other interventions to one or more human subjects? 4. What type of study or clinical trial is required or agreed upon (describe and check type below)? If the study or trial will be performed in a subpopulation, list here. An oral toxicity study with netupitant alone of at least 8 weeks duration in neonatal rats is needed. This study should include evaluation of developmental parameters, neurobehavioral effects, and fertility. Required Observational pharmacoepidemiologic study Registry studies Primary safety study or clinical trial Pharmacogenetic or pharmacogenomic study or clinical trial if required to further assess safety Thorough Q-T clinical trial Nonclinical (animal) safety study (e.g., carcinogenicity, reproductive toxicology) Nonclinical study (laboratory resistance, receptor affinity, quality study related to safety) Pharmacokinetic studies or clinical trials Drug interaction or bioavailability studies or clinical trials Dosing trials PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 2 of 3 Continuation of Question 4 Additional data or analysis required for a previously submitted or expected study/clinical trial (provide explanation) Meta-analysis or pooled analysis of previous studies/clinical trials Immunogenicity as a marker of safety Other (provide explanation) Agreed upon: Quality study without a safety endpoint (e.g., manufacturing, stability) Pharmacoepidemiologic study not related to safe drug use (e.g., natural history of disease, background rates of adverse events) Clinical trials primarily designed to further define efficacy (e.g., in another condition, different disease severity, or subgroup) that are NOT required under Subpart H/E Dose-response study or clinical trial performed for effectiveness Nonclinical study, not safety-related (specify) Other 5. Is the PMR/PMC clear, feasible, and appropriate? Does the study/clinical trial meet criteria for PMRs or PMCs? Are the objectives clear from the description of the PMR/PMC? Has the applicant adequately justified the choice of schedule milestone dates? Has the applicant had sufficient time to review the PMRs/PMCs, ask questions, determine feasibility, and contribute to the development process? Check if this form describes a FDAAA PMR that is a randomized controlled clinical trial If so, does the clinical trial meet the following criteria? There is a significant question about the public health risks of an approved drug There is not enough existing information to assess these risks Information cannot be gained through a different kind of investigation The trial will be appropriately designed to answer question about a drug’s efficacy and safety, and The trial will emphasize risk minimization for participants as the protocol is developed PMR/PMC Development Coordinator: This PMR/PMC has been reviewed for clarity and consistency, and is necessary to further refine the safety, efficacy, or optimal use of a drug, or to ensure consistency and reliability of drug quality. _______________________________________ (signature line for BLAs) PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 3 of 3 PMR/PMC Development Template This template should be completed by the PMR/PMC Development Coordinator and included for each PMR/PMC in the Action Package. NDA/BLA # Product Name: NDA 205718 Akynzeo (netupitant + palonosetron fixed dose combination) Capsule PMR/PMC Description: A PK/PD dose finding study of netupitant to characterize netupitant PK/PD relationship for complete response in the delayed phase following oral administration of single dose of netupitant given concomitantly (in separate formulations) with oral single administration of palonosetron in pediatric cancer patients ages 0 to17 years undergoing treatment with emetogenic chemotherapy including highly emetogenic chemotherapy. You must conduct this study with an age appropriate formulation. PMR/PMC Schedule Milestones: Final Protocol Submission: Study/Trial Completion: Final Report Submission: 11/01/2015 04/30/2018 09/30/2018 1. During application review, explain why this issue is appropriate for a PMR/PMC instead of a pre-approval requirement. Check type below and describe. Unmet need Life-threatening condition Long-term data needed Only feasible to conduct post-approval Prior clinical experience indicates safety Small subpopulation affected Theoretical concern Other The sponsor will need to develop an age appropriate formulation of netupitant alone to administer with IV Aloxi, given orally, for use in pediatric patients. Only after the age appropriate formulation of netupitant alone is developed and found suitable for use can the PK/PD study commence. The timeline for final protocol submission must allow sufficient time for the sponsor to develop the netupitant formulation. 2. Describe the particular review issue and the goal of the study/clinical trial. If the study/clinical trial is a FDAAA PMR, describe the risk. If the FDAAA PMR is created post-approval, describe the “new safety information.” PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 1 of 4 Study #1 is planned to be a PK/PD study in pediatric cancer patients to characterize netupitant PK/PD relationship when administered concomitantly with the approved dose of palonosetron. The PD parameter to be measured is complete response. Doses for both drugs are planned to be based on body weight from 0 to 17 years of age in patients undergoing treatment with emetogenic chemotherapy. Based and contingent upon formulation development outcomes, an age appropriate oral formulation of netupitant-alone will be used and it will be administered concomitantly with I.V. Aloxi given orally. The acceptability of the oral use of I.V. Aloxi in pediatric cancer patients was already agreed with FDA for the Written Request program of Aloxi NDA 21372. 3. If the study/clinical trial is a PMR, check the applicable regulation. If not a PMR, skip to 4. - Which regulation? Accelerated Approval (subpart H/E) Animal Efficacy Rule Pediatric Research Equity Act FDAAA required safety study/clinical trial - If the PMR is a FDAAA safety study/clinical trial, does it: (check all that apply) Assess a known serious risk related to the use of the drug? Assess signals of serious risk related to the use of the drug? Identify an unexpected serious risk when available data indicate the potential for a serious risk? - If the PMR is a FDAAA safety study/clinical trial, will it be conducted as: Analysis of spontaneous postmarketing adverse events? Do not select the above study/clinical trial type if: such an analysis will not be sufficient to assess or identify a serious risk Analysis using pharmacovigilance system? Do not select the above study/clinical trial type if: the new pharmacovigilance system that the FDA is required to establish under section 505(k)(3) has not yet been established and is thus not sufficient to assess this known serious risk, or has been established but is nevertheless not sufficient to assess or identify a serious risk Study: all other investigations, such as investigations in humans that are not clinical trials as defined below (e.g., observational epidemiologic studies), animal studies, and laboratory experiments? Do not select the above study type if: a study will not be sufficient to identify or assess a serious risk Clinical trial: any prospective investigation in which the sponsor or investigator determines the method of assigning investigational product or other interventions to one or more human subjects? 4. What type of study or clinical trial is required or agreed upon (describe and check type below)? If the study or trial will be performed in a subpopulation, list here. PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 2 of 4 Required Observational pharmacoepidemiologic study Registry studies Primary safety study or clinical trial Pharmacogenetic or pharmacogenomic study or clinical trial if required to further assess safety Thorough Q-T clinical trial Nonclinical (animal) safety study (e.g., carcinogenicity, reproductive toxicology) Nonclinical study (laboratory resistance, receptor affinity, quality study related to safety) Pharmacokinetic studies or clinical trials Drug interaction or bioavailability studies or clinical trials Dosing trials Continuation of Question 4 Additional data or analysis required for a previously submitted or expected study/clinical trial (provide explanation) Meta-analysis or pooled analysis of previous studies/clinical trials Immunogenicity as a marker of safety Other (provide explanation) Agreed upon: Quality study without a safety endpoint (e.g., manufacturing, stability) Pharmacoepidemiologic study not related to safe drug use (e.g., natural history of disease, background rates of adverse events) Clinical trials primarily designed to further define efficacy (e.g., in another condition, different disease severity, or subgroup) that are NOT required under Subpart H/E Dose-response study or clinical trial performed for effectiveness Nonclinical study, not safety-related (specify) Other 5. Is the PMR/PMC clear, feasible, and appropriate? Does the study/clinical trial meet criteria for PMRs or PMCs? Are the objectives clear from the description of the PMR/PMC? Has the applicant adequately justified the choice of schedule milestone dates? Has the applicant had sufficient time to review the PMRs/PMCs, ask questions, determine feasibility, and contribute to the development process? Check if this form describes a FDAAA PMR that is a randomized controlled clinical trial If so, does the clinical trial meet the following criteria? There is a significant question about the public health risks of an approved drug PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 3 of 4 There is not enough existing information to assess these risks Information cannot be gained through a different kind of investigation The trial will be appropriately designed to answer question about a drug’s efficacy and safety, and The trial will emphasize risk minimization for participants as the protocol is developed PMR/PMC Development Coordinator: This PMR/PMC has been reviewed for clarity and consistency, and is necessary to further refine the safety, efficacy, or optimal use of a drug, or to ensure consistency and reliability of drug quality. _______________________________________ (signature line for BLAs) PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 4 of 4 PMR/PMC Development Template This template should be completed by the PMR/PMC Development Coordinator and included for each PMR/PMC in the Action Package. NDA/BLA # Product Name: NDA 205718 Akynzeo (netupitant + palonosetron FDC) capsules PMR/PMC Description: An adequate, well-controlled, double-blind, randomized, study to evaluate the safety and efficacy of a dose of the netupitant-palonosetron fixed dose combination compared to standard therapy in pediatric cancer patients ages 0 to 17 years undergoing treatment with emetogenic chemotherapy including highly emetogenic chemotherapy. You must conduct this study with an age appropriate formulation. PMR/PMC Schedule Milestones: Final Protocol Submission: Study/Trial Completion: Final Report Submission: 04/30/2019 12/31/2021 04/30/2022 1. During application review, explain why this issue is appropriate for a PMR/PMC instead of a pre-approval requirement. Check type below and describe. Unmet need Life-threatening condition Long-term data needed Only feasible to conduct post-approval Prior clinical experience indicates safety Small subpopulation affected Theoretical concern Other PREA required safety and efficacy trial 2. Describe the particular review issue and the goal of the study/clinical trial. If the study/clinical trial is a FDAAA PMR, describe the risk. If the FDAAA PMR is created post-approval, describe the “new safety information.” PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 1 of 4 The goal of the trial is to obtain safety and efficacy data in order to inform labeling for pediatric use. 3. If the study/clinical trial is a PMR, check the applicable regulation. If not a PMR, skip to 4. - Which regulation? Accelerated Approval (subpart H/E) Animal Efficacy Rule Pediatric Research Equity Act FDAAA required safety study/clinical trial - If the PMR is a FDAAA safety study/clinical trial, does it: (check all that apply) Assess a known serious risk related to the use of the drug? Assess signals of serious risk related to the use of the drug? Identify an unexpected serious risk when available data indicate the potential for a serious risk? - If the PMR is a FDAAA safety study/clinical trial, will it be conducted as: Analysis of spontaneous postmarketing adverse events? Do not select the above study/clinical trial type if: such an analysis will not be sufficient to assess or identify a serious risk Analysis using pharmacovigilance system? Do not select the above study/clinical trial type if: the new pharmacovigilance system that the FDA is required to establish under section 505(k)(3) has not yet been established and is thus not sufficient to assess this known serious risk, or has been established but is nevertheless not sufficient to assess or identify a serious risk Study: all other investigations, such as investigations in humans that are not clinical trials as defined below (e.g., observational epidemiologic studies), animal studies, and laboratory experiments? Do not select the above study type if: a study will not be sufficient to identify or assess a serious risk Clinical trial: any prospective investigation in which the sponsor or investigator determines the method of assigning investigational product or other interventions to one or more human subjects? 4. What type of study or clinical trial is required or agreed upon (describe and check type below)? If the study or trial will be performed in a subpopulation, list here. An adequate, well-controlled, double-blind, randomized, study to evaluate the safety and efficacy of a dose of the netupitant-palonosetron FDC compared to standard therapy in pediatric cancer patients from 0 to17 years of age undergoing treatment with emetogenic chemotherapy. Study #2 is planned to be an add-on superiority trial of the FDC versus vs. palonosetron, or a non-inferiority study of the FDC versus aprepitant used withpalonosetron. The final age appropriate pediatric oral formulation of the netupitant + palonosetron FDC is planned to be used in this trial. PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 2 of 4 Required Observational pharmacoepidemiologic study Registry studies Primary safety study or clinical trial Pharmacogenetic or pharmacogenomic study or clinical trial if required to further assess safety Thorough Q-T clinical trial Nonclinical (animal) safety study (e.g., carcinogenicity, reproductive toxicology) Nonclinical study (laboratory resistance, receptor affinity, quality study related to safety) Pharmacokinetic studies or clinical trials Drug interaction or bioavailability studies or clinical trials Dosing trials Continuation of Question 4 Additional data or analysis required for a previously submitted or expected study/clinical trial (provide explanation) Meta-analysis or pooled analysis of previous studies/clinical trials Immunogenicity as a marker of safety Other (provide explanation) PREA Efficacy and Safety Study Agreed upon: Quality study without a safety endpoint (e.g., manufacturing, stability) Pharmacoepidemiologic study not related to safe drug use (e.g., natural history of disease, background rates of adverse events) Clinical trials primarily designed to further define efficacy (e.g., in another condition, different disease severity, or subgroup) that are NOT required under Subpart H/E Dose-response study or clinical trial performed for effectiveness Nonclinical study, not safety-related (specify) Other 5. Is the PMR/PMC clear, feasible, and appropriate? Does the study/clinical trial meet criteria for PMRs or PMCs? Are the objectives clear from the description of the PMR/PMC? Has the applicant adequately justified the choice of schedule milestone dates? Has the applicant had sufficient time to review the PMRs/PMCs, ask questions, determine feasibility, and contribute to the development process? Check if this form describes a FDAAA PMR that is a randomized controlled clinical trial If so, does the clinical trial meet the following criteria? There is a significant question about the public health risks of an approved drug There is not enough existing information to assess these risks Information cannot be gained through a different kind of investigation The trial will be appropriately designed to answer question about a drug’s efficacy and safety, and The trial will emphasize risk minimization for participants as the protocol is developed PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 3 of 4 PMR/PMC Development Coordinator: This PMR/PMC has been reviewed for clarity and consistency, and is necessary to further refine the safety, efficacy, or optimal use of a drug, or to ensure consistency and reliability of drug quality. _______________________________________ (signature line for BLAs) PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 4 of 4 PMR/PMC Development Template This template should be completed by the PMR/PMC Development Coordinator and included for each PMR/PMC in the Action Package. NDA/BLA # Product Name: NDA 205718 Akynzeo® (netupitant-palonosetron hydrochloride) Capsule PMR/PMC Description: In-vivo drug interaction study to evaluate the duration of inhibitory effects of AKYNZEO on CYP3A4 enzyme activity beyond 4 days after AKYNZEO administration PMR/PMC Schedule Milestones: Final Protocol Submission: Study/Trial Completion: Final Report Submission: 01/31/2015 01/31/2016 06/30/2016 1. During application review, explain why this issue is appropriate for a PMR/PMC instead of a pre-approval requirement. Check type below and describe. Unmet need Life-threatening condition Long-term data needed Only feasible to conduct post-approval Prior clinical experience indicates safety Small subpopulation affected Theoretical concern Other The sponsor conducted two drug interaction studies to address the inhibition of CYP3A4 enzyme activity by netupitant. Nevertheless, it was found that the information was insufficient to fully characterize the duration of CYP3A4 enzyme inhibition. The estimation based on in-vitro assays suggest that drug interaction is possible even on Day 6 after single dose administration of netupitant, a component of Akynzeo. Therefore, an additional study is being committed to confirm the estimation as well as the worst case scenario. In the meantime, the labeling will state the observed drug interaction via inhibition of CYP3A4 as well as the duration of such inhibition at least for 4 days based on study results. 2. Describe the particular review issue and the goal of the study/clinical trial. If the study/clinical trial is a FDAAA PMR, describe the risk. If the FDAAA PMR is created post-approval, describe the “new safety information.” Co-administration of a single dose of netupitant increased the exposure to dexamethasone, a substrate of CYP3A4 by 1.7-fold on Day 1 and up to 2.4-fold on Day 2 and Day 4. The potential inhibitory effect of netupitant on CYP3A4 was not studied beyond Day 4. Given AKYNZEO will be used in patients who require multiple medications for underlying disease treatment as well as supportive care, a study is necessary to provide adequate information for use of AKYNZEO with concomitant medications that are CYP3A4 substrates. PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 1 of 4 3. If the study/clinical trial is a PMR, check the applicable regulation. If not a PMR, skip to 4. - Which regulation? Accelerated Approval (subpart H/E) Animal Efficacy Rule Pediatric Research Equity Act FDAAA required safety study/clinical trial - If the PMR is a FDAAA safety study/clinical trial, does it: (check all that apply) Assess a known serious risk related to the use of the drug? Assess signals of serious risk related to the use of the drug? Identify an unexpected serious risk when available data indicate the potential for a serious risk? - If the PMR is a FDAAA safety study/clinical trial, will it be conducted as: Analysis of spontaneous postmarketing adverse events? Do not select the above study/clinical trial type if: such an analysis will not be sufficient to assess or identify a serious risk Analysis using pharmacovigilance system? Do not select the above study/clinical trial type if: the new pharmacovigilance system that the FDA is required to establish under section 505(k)(3) has not yet been established and is thus not sufficient to assess this known serious risk, or has been established but is nevertheless not sufficient to assess or identify a serious risk Study: all other investigations, such as investigations in humans that are not clinical trials as defined below (e.g., observational epidemiologic studies), animal studies, and laboratory experiments? Do not select the above study type if: a study will not be sufficient to identify or assess a serious risk Clinical trial: any prospective investigation in which the sponsor or investigator determines the method of assigning investigational product or other interventions to one or more human subjects? 4. What type of study or clinical trial is required or agreed upon (describe and check type below)? If the study or trial will be performed in a subpopulation, list here. The study design will include healthy subjects who will receive a regimen of dexamethasone alone administered for up to 6 days and beyond (Treatment A) and the same regimen of dexamethasone plus AKYNZEO on day 1 only (Treatment B), according to a two-period, two-sequence, randomized crossover design. The PK profile of dexamethasone will be fully described on different days throughout the study duration, with/without the single AKYNZEO administration. The PK profile of netupitant and its metabolites M1, M2 and M3 will also be followed in parallel. Data analysis will primarily compare the AUCτ of dexamethasone with/ without netupitant co-administration, in order to determine the duration of CYP3A4 inhibition. Additional analysis will consider the ratios of trough dexamethasone concentrations over time with / without netupitant co-administration. Required Observational pharmacoepidemiologic study Registry studies PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 2 of 4 Primary safety study or clinical trial Pharmacogenetic or pharmacogenomic study or clinical trial if required to further assess safety Thorough Q-T clinical trial Nonclinical (animal) safety study (e.g., carcinogenicity, reproductive toxicology) Nonclinical study (laboratory resistance, receptor affinity, quality study related to safety) Pharmacokinetic studies or clinical trials Drug interaction or bioavailability studies or clinical trials Dosing trials Continuation of Question 4 Additional data or analysis required for a previously submitted or expected study/clinical trial (provide explanation) Meta-analysis or pooled analysis of previous studies/clinical trials Immunogenicity as a marker of safety Other (provide explanation) Agreed upon: Quality study without a safety endpoint (e.g., manufacturing, stability) Pharmacoepidemiologic study not related to safe drug use (e.g., natural history of disease, background rates of adverse events) Clinical trials primarily designed to further define efficacy (e.g., in another condition, different disease severity, or subgroup) that are NOT required under Subpart H/E Dose-response study or clinical trial performed for effectiveness Nonclinical study, not safety-related (specify) Other In vivo drug interaction study in healthy subjects 5. Is the PMR/PMC clear, feasible, and appropriate? Does the study/clinical trial meet criteria for PMRs or PMCs? Are the objectives clear from the description of the PMR/PMC? Has the applicant adequately justified the choice of schedule milestone dates? Has the applicant had sufficient time to review the PMRs/PMCs, ask questions, determine feasibility, and contribute to the development process? Check if this form describes a FDAAA PMR that is a randomized controlled clinical trial If so, does the clinical trial meet the following criteria? There is a significant question about the public health risks of an approved drug There is not enough existing information to assess these risks Information cannot be gained through a different kind of investigation The trial will be appropriately designed to answer question about a drug’s efficacy and safety, and The trial will emphasize risk minimization for participants as the protocol is developed PMR/PMC Development Coordinator: This PMR/PMC has been reviewed for clarity and consistency, and is necessary to further refine the safety, efficacy, or optimal use of a drug, or to ensure consistency and reliability of drug quality. PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 3 of 4 _______________________________________ (signature line for BLAs) Appears This Way On Original PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 4 of 4 PMR/PMC Development Template This template should be completed by the PMR/PMC Development Coordinator and included for each PMR/PMC in the Action Package. NDA/BLA # Product Name: NDA 205718 Akynzeo® (netupitant-palonosetron hydrochloride) Capsule PMR/PMC Description: In-vitro study to evaluate the potential of netupitant being a substrate for P-gp transporter in a bi-directional transport assay system. PMR/PMC Schedule Milestones: Final Report Submission: 10/31/2014 1. During application review, explain why this issue is appropriate for a PMR/PMC instead of a pre-approval requirement. Check type below and describe. Unmet need Life-threatening condition Long-term data needed Only feasible to conduct post-approval Prior clinical experience indicates safety Small subpopulation affected Theoretical concern Other The sponsor did not adequately evaluate the potential of netupitant (a component of Akynzeo) being a substrate of P-gp. In the meantime, the labeling will state that the potential of netupitant being a substrate for P-gp is unknown. 2. Describe the particular review issue and the goal of the study/clinical trial. If the study/clinical trial is a FDAAA PMR, describe the risk. If the FDAAA PMR is created post-approval, describe the “new safety information.” The potential of netupitant being a substrate for P-gp in ATPase activation assay suggested that netupitant is likely a substrate for P-gp. However, information is lacking whether netupitant is a substrate for P-gp on bi-directional transport assay system, which is considered a confirmatory study. PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 1 of 3 3. If the study/clinical trial is a PMR, check the applicable regulation. If not a PMR, skip to 4. - Which regulation? Accelerated Approval (subpart H/E) Animal Efficacy Rule Pediatric Research Equity Act FDAAA required safety study/clinical trial - If the PMR is a FDAAA safety study/clinical trial, does it: (check all that apply) Assess a known serious risk related to the use of the drug? Assess signals of serious risk related to the use of the drug? Identify an unexpected serious risk when available data indicate the potential for a serious risk? - If the PMR is a FDAAA safety study/clinical trial, will it be conducted as: Analysis of spontaneous postmarketing adverse events? Do not select the above study/clinical trial type if: such an analysis will not be sufficient to assess or identify a serious risk Analysis using pharmacovigilance system? Do not select the above study/clinical trial type if: the new pharmacovigilance system that the FDA is required to establish under section 505(k)(3) has not yet been established and is thus not sufficient to assess this known serious risk, or has been established but is nevertheless not sufficient to assess or identify a serious risk Study: all other investigations, such as investigations in humans that are not clinical trials as defined below (e.g., observational epidemiologic studies), animal studies, and laboratory experiments? Do not select the above study type if: a study will not be sufficient to identify or assess a serious risk Clinical trial: any prospective investigation in which the sponsor or investigator determines the method of assigning investigational product or other interventions to one or more human subjects? 4. What type of study or clinical trial is required or agreed upon (describe and check type below)? If the study or trial will be performed in a subpopulation, list here. Assessment of potential interaction of netupitant with P-gp as substrate will be based on the bidirectional transport methodology and utilize polarized monolayer cells as the functional assay. Bi-directional transport will be performed in human colon adenocarcinoma (Caco-2) cells seeded on polycarbonate microporous membrane filters. Apparent Permeability Coefficient (Papp) in cm⋅10-6 /sec and efflux ratio value will be determined. Standard compound included in each permeability assay are: Digoxin, as P-gp substrate, Cyclosporine A and Verapamil, as P-gp inhibitors. Required Observational pharmacoepidemiologic study Registry studies Primary safety study or clinical trial Pharmacogenetic or pharmacogenomic study or clinical trial if required to further assess safety Thorough Q-T clinical trial PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 2 of 3 Nonclinical (animal) safety study (e.g., carcinogenicity, reproductive toxicology) Nonclinical study (laboratory resistance, receptor affinity, quality study related to safety) Pharmacokinetic studies or clinical trials Drug interaction or bioavailability studies or clinical trials Dosing trials Continuation of Question 4 Additional data or analysis required for a previously submitted or expected study/clinical trial (provide explanation) Meta-analysis or pooled analysis of previous studies/clinical trials Immunogenicity as a marker of safety Other (provide explanation) Agreed upon: Quality study without a safety endpoint (e.g., manufacturing, stability) Pharmacoepidemiologic study not related to safe drug use (e.g., natural history of disease, background rates of adverse events) Clinical trials primarily designed to further define efficacy (e.g., in another condition, different disease severity, or subgroup) that are NOT required under Subpart H/E Dose-response study or clinical trial performed for effectiveness Nonclinical study, not safety-related (specify) Other In vitro study 5. Is the PMR/PMC clear, feasible, and appropriate? Does the study/clinical trial meet criteria for PMRs or PMCs? Are the objectives clear from the description of the PMR/PMC? Has the applicant adequately justified the choice of schedule milestone dates? Has the applicant had sufficient time to review the PMRs/PMCs, ask questions, determine feasibility, and contribute to the development process? Check if this form describes a FDAAA PMR that is a randomized controlled clinical trial If so, does the clinical trial meet the following criteria? There is a significant question about the public health risks of an approved drug There is not enough existing information to assess these risks Information cannot be gained through a different kind of investigation The trial will be appropriately designed to answer question about a drug’s efficacy and safety, and The trial will emphasize risk minimization for participants as the protocol is developed PMR/PMC Development Coordinator: This PMR/PMC has been reviewed for clarity and consistency, and is necessary to further refine the safety, efficacy, or optimal use of a drug, or to ensure consistency and reliability of drug quality. _______________________________________ (signature line for BLAs) PMR/PMC Development Template Reference ID: 3624989 Last Updated 9/10/2014 Page 3 of 3 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------MARY H CHUNG 09/10/2014 RUYI HE 09/10/2014 Reference ID: 3624989 MEMORANDUM Department of Health and Human Services Food and Drug Administration Center for Drug Evaluation and Research Date: August 4, 2014 To: Donna Griebel, M.D., Director Division of Gastroenterology and Inborn Error Products Through: Michael Klein, Ph.D., Director Silvia Calderon, Ph.D., Team Leader Controlled Substance Staff (CSS) From: Katherine Bonson, Ph.D., Pharmacologist Controlled Substance Staff Subject: Statement on Section 9.0 of drug label Akynzeo (Netupitant and Palonosetron HCI Fixed-Dose Combination Capsule) NDA 205,718 (IND 73,493) Indication: Prevention of acute and delayed nausea and vomiting associated with cancer chemotherapy Sponsor: Helsinn Healthcare, SA PDUFA Goal Date: September 26, 2014 Background This memorandum responds to a request by the Division of Gastroenterology and Inborn Error Products to evaluate a proposal from Helsinn Healthcare on August 1, 2014 to exclude Section 9.0 (Drug Abuse and Dependence) from the drug label for Akynzeo (Netupitant and Palonosetron HCI Fixed-Dose Combination Capsule). The Sponsor states that their proposal is supported by a statement in the FDA Guidance for Industry: Labeling for Human Prescription Drug and Biological Products – Implementing the PLR Content and Format Requirements (2013) that, “The Drug Abuse and Dependence section should be omitted for a drug that is not a controlled substance and has no potential for abuse or dependence.” CSS previously concluded in our May 30, 2014, consult that Akynzeo has no potential for abuse or dependence. 1 of 2 Reference ID: 3604389 Netupitant + Palonosetron (Akynzeo) NDA 205,718 Conclusion and Recommendation CSS accepts the Sponsor’s proposal to eliminate Section 9.0 from the drug label for Akynzeo, based on the Guidance for Industry: Labeling for Human Prescription Drug and Biological Products – Implementing the PLR Content and Format Requirements (2013). This recommendation replaces our previous recommendation in our May 30, 2014, consult that the drug label should include brief information in Section 9.0 about abuserelated study data showing that netupitant + palonosetron has no potential for abuse or dependence. 2 Reference ID: 3604389 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------KATHERINE R BONSON 08/04/2014 SILVIA N CALDERON 08/04/2014 MICHAEL KLEIN 08/04/2014 Reference ID: 3604389 REGULATORY PROJECT MANAGER PHYSICIAN’S LABELING RULE (PLR) FORMAT REVIEW OF THE PRESCRIBING INFORMATION Complete for all new NDAs, BLAs, Efficacy Supplements, and PLR Conversion Labeling Supplements Application: NDA 205718 Application Type: New NDA Name of Drug/Dosage Form: Akynzeo (netupitant/palonosetron HCl) fixed-dose combination capsule Applicant: Helsinn Healthcare, Inc. Receipt Date: September 27, 2013 Goal Date: September 26, 2014 1. Regulatory History and Applicant’s Main Proposals On September 15, 2006, Helsinn Healthcare submitted IND 73493 for netupitant/ palonosetron fixed-dose combination capsules for treatment of chemotherapy induced nausea and vomiting. Helsinn’s clinical development program was discussed at the end-of-phase 2 meeting held on July 20, 2009. A series of Special Protocol Assessment (SPA) requests were submitted by the sponsor and Type A SPA meetings were held January 22, 2010 and July 15, 2010. Per discussion from these meetings, four clinical studies (NETU-07-07, PALO-10-01, NETU-08-18, and NETU-10-29) were conducted to support the efficacy and safety of the fixed-dose combination capsule for the prevention of acute and delayed phases of CINV-HEC and CINVMEC. On April 16, 2013, a pre-NDA meeting was held to discuss the results of the phase 3 trials, the content and format of the planned eCTD NDA submission, proposed labeling and the schedule to submit the pediatric study plan. On September 27, 2013, Helsinn Healthcare submitted NDA 205718 for the following indications: 1. Prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of highly emetogenic cancer chemotherapy (CINV HEC). 2. Prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of moderately emetogenic cancer chemotherapy (CINV MEC). 2. Review of the Prescribing Information This review is based on the applicant’s submitted Word format of the prescribing information (PI). The applicant’s proposed PI was reviewed in accordance with the labeling format requirements listed in the “Selected Requirements for Prescribing Information (SRPI)” checklist (see the Appendix). 3. Conclusions/Recommendations SRPI format deficiencies were identified in the review of this PI. For a list of these deficiencies see the Appendix. Reference ID: 3604386 Selected Requirements of Prescribing Information All SRPI format deficiencies of the PI will be conveyed to the applicant in the 74-day letter/an advice letter. The applicant will be asked to correct these deficiencies and resubmit the PI in Word format by January 6, 2014. The resubmitted PI will be used for further labeling review. Appendix The Selected Requirement of Prescribing Information (SRPI) is a 42-item, drop-down checklist of important format elements of the prescribing information (PI) based on labeling regulations (21 CFR 201.56 and 201.57) and guidances. Highlights See Appendix A for a sample tool illustrating the format for the Highlights. HIGHLIGHTS GENERAL FORMAT and HORIZONTAL LINES IN THE PI YES NO 1. Highlights (HL) must be in a minimum of 8-point font and should be in two-column format, with ½ inch margins on all sides and between columns. Comment: 2. The length of HL must be one-half page or less (the HL Boxed Warning does not count against the one-half page requirement) unless a waiver has been granted in a previous submission (e.g., the application being reviewed is an efficacy supplement). Instructions to complete this item: If the length of the HL is one-half page or less, then select “YES” in the drop-down menu because this item meets the requirement. However, if HL is longer than one-half page:  For the Filing Period: • For efficacy supplements: If a waiver was previously granted, select “YES” in the dropdown menu because this item meets the requirement. • For NDAs/BLAs and PLR conversions: Select “NO” because this item does not meet the requirement (deficiency). The RPM notifies the Cross-Discipline Team Leader (CDTL) of the excessive HL length and the CDTL determines if this deficiency is included in the 74day or advice letter to the applicant.  For the End-of-Cycle Period: • Select “YES” in the drop down menu if a waiver has been previously (or will be) granted by the review division in the approval letter and document that waiver was (or will be) granted. Comment: Highlights must be one-half page or less unless a waiver has been granted in a previous submission. YES 3. A horizontal line must separate HL from the Table of Contents (TOC). A horizontal line must separate the TOC from the FPI. Comment: SRPI version 3: October 2013 Reference ID: 3604386 Page 2 of 10 Selected Requirements of Prescribing Information YES 4. All headings in HL must be bolded and presented in the center of a horizontal line (each horizontal line should extend over the entire width of the column as shown in Appendix A). The headings should be in UPPER CASE letters. Comment: 5. White space should be present before each major heading in HL. There must be no white space between the HL Heading and HL Limitation Statement. There must be no white space between the product title and Initial U.S. Approval. See Appendix A for a sample tool illustrating white space in HL. Comment: 6. Each summarized statement or topic in HL must reference the section(s) or subsection(s) of the Full Prescribing InfOImation (FPI) that contain more detailed inf01mation. The preferred f01mat is the numerical identi?er in parenthesis at the end of each smnmarized statement or topic. Comment: YES 7. Section headings must be presented in the following order in HL: Section Required/Optional 0 Highlights Heading Required 0 Highlights Limitation Statement Required 0 Product Title Required 0 Initial U.S. Approval Required 0 Boxed Warning Required if a BOXED WARNING is in the FPI 0 Recent Major Changes Required for only certain changes to 0 Indications and Usage Required Dosage and Administration Required Dosage Forms and Required Contraindications Required (if no contraindications must state ?None.?) 0 Warnings and Precautions Not required by regulation, but should be present Adverse Reactions Required 0 Drug Interactions Optional 0 Use in Specific Populations Optional 0 Patient Counseling Information Statement Required 0 Revision Date Required RMC only applies to the BOXED WARNING. INDICATIONS AND USAGE. DOSAGE AND ADIVIINISTRATION. CONTRAINDICATIONS. and WARNINGS AND PRECAUTIONS sections. Comment: HIGHLIGHTS DETAILS Highlights Heading 8. At the beginning of HL, the following heading must be bolded and should appear in all UPPER CASE letters: OF PRESCRIBING Comment: Highlights Limitation Statement YES 9. The bolded HL Limitation Statement must include the following verbatim statement: ?These highlights do not include all the information needed to use (insert name of drug product) SRPI version 3: October 2013 Reference ID: 3604386 Page 3 of 10 Selected Requirements of Prescribing Information safely and effectively. See full prescribing information for (insert name of drug product).” The name of drug product should appear in UPPER CASE letters. Comment: Product Title in Highlights YES 10. Product title must be bolded. Comment: Initial U.S. Approval in Highlights YES 11. Initial U.S. Approval in HL must be bolded, and include the verbatim statement “Initial U.S. Approval:” followed by the 4-digit year. Comment: N/A N/A N/A N/A N/A N/A Boxed Warning (BW) in Highlights 12. All text in the BW must be bolded. Comment: 13. The BW must have a heading in UPPER CASE, containing the word “WARNING” (even if more than one warning, the term, “WARNING” and not “WARNINGS” should be used) and other words to identify the subject of the warning (e.g., “WARNING: SERIOUS INFECTIONS and ACUTE HEPATIC FAILURE”). The BW heading should be centered. Comment: 14. The BW must always have the verbatim statement “See full prescribing information for complete boxed warning.” This statement should be centered immediately beneath the heading and appear in italics. Comment: 15. The BW must be limited in length to 20 lines (this includes white space but does not include the BW heading and the statement “See full prescribing information for complete boxed warning.”). Comment: Recent Major Changes (RMC) in Highlights 16. RMC pertains to only the following five sections of the FPI: BOXED WARNING, INDICATIONS AND USAGE, DOSAGE AND ADMINISTRATION, CONTRAINDICATIONS, and WARNINGS AND PRECAUTIONS. RMC must be listed in the same order in HL as the modified text appears in FPI. Comment: 17. The RMC must include the section heading(s) and, if appropriate, subsection heading(s) affected by the recent major change, together with each section’s identifying number and date (month/year format) on which the change was incorporated in the PI (supplement approval date). For example, “Warnings and Precautions, Acute Liver Failure (5.1) --- 9/2013”. Comment: N/A SRPI version 3: October 2013 Reference ID: 3604386 Page 4 of 10 Selected Requirements of Prescribing Information 18. The RMC must list changes for at least one year after the supplement is approved and must be removed at the first printing subsequent to one year (e.g., no listing should be one year older than revision date). Comment: YES N/A YES YES Indications and Usage in Highlights 19. If a product belongs to an established pharmacologic class, the following statement is required under the Indications and Usage heading in HL: “(Product) is a (name of established pharmacologic class) indicated for (indication)”. Comment: Dosage Forms and Strengths in Highlights 20. For a product that has several dosage forms (e.g., capsules, tablets, and injection), bulleted subheadings or tabular presentations of information should be used under the Dosage Forms and Strengths heading. Comment: Contraindications in Highlights 21. All contraindications listed in the FPI must also be listed in HL or must include the statement “None” if no contraindications are known. Each contraindication should be bulleted when there is more than one contraindication. Comment: Adverse Reactions in Highlights 22. For drug products other than vaccines, the verbatim bolded statement must be present: “To report SUSPECTED ADVERSE REACTIONS, contact (insert name of manufacturer) at (insert manufacturer’s U.S. phone number) or FDA at 1-800-FDA-1088 or www.fda.gov/medwatch”. Comment: Patient Counseling Information Statement in Highlights YES 23. The Patient Counseling Information statement must include one of the following three bolded verbatim statements that is most applicable: If a product does not have FDA-approved patient labeling: • “See 17 for PATIENT COUNSELING INFORMATION” If a product has FDA-approved patient labeling: • “See 17 for PATIENT COUNSELING INFORMATION and FDA-approved patient labeling” • “See 17 for PATIENT COUNSELING INFORMATION and Medication Guide” Comment: YES Revision Date in Highlights 24. The revision date must be at the end of HL, and should be bolded and right justified (e.g., “Revised: 9/2013”). SRPI version 3: October 2013 Reference ID: 3604386 Page 5 of 10 Selected Requirements of Prescribing Information Comment: Contents: Table of Contents (TOC) See Appendix A for a sample tool illustrating the format for the Table of Contents. NO YES N/A YES NO NO YES 25. The TOC should be in a two-column format. Comment: The Table of Content (TOC) should be in a two-column format. 26. The following heading must appear at the beginning of the TOC: “FULL PRESCRIBING INFORMATION: CONTENTS”. This heading should be in all UPPER CASE letters and bolded. Comment: 27. The same heading for the BW that appears in HL and the FPI must also appear at the beginning of the TOC in UPPER CASE letters and bolded. Comment: 28. In the TOC, all section headings must be bolded and should be in UPPER CASE. Comment: 29. In the TOC, all subsection headings must be indented and not bolded. The headings should be in title case [first letter of all words are capitalized except first letter of prepositions (through), articles (a, an, and the), or conjunctions (for, and)]. Comment: The subsection headings are indented but bolded. The word “action” in subsection 12.1 must be capitalized. 30. The section and subsection headings in the TOC must match the section and subsection headings in the FPI. Comment: The numbers 9 and 15 must be deleted from the TOC. 31. In the TOC, when a section or subsection is omitted, the numbering must not change. If a section or subsection from 201.56(d)(1) is omitted from the FPI and TOC, the heading “FULL PRESCRIBING INFORMATION: CONTENTS” must be followed by an asterisk and the following statement must appear at the end of TOC: “*Sections or subsections omitted from the full prescribing information are not listed.” Comment: SRPI version 3: October 2013 Reference ID: 3604386 Page 6 of 10 Selected Requirements of Prescribing Information Full Prescribing Information (FPI) FULL PRESCRIBING INFORMATION: GENERAL FORMAT YES 32. The bolded section and subsection headings in the FPI must be named and numbered in accordance with 21 CFR 201.56(d)(1) as noted below (section and subsection headings should be in UPPER CASE and title case, respectively). If a section/subsection required by regulation is omitted, the numbering must not change. Additional subsection headings (i.e., those not named by regulation) must also be bolded and numbered. BOXED WARNING 1 INDICATIONS AND USAGE 2 DOSAGE AND ADMINISTRATION 3 DOSAGE FORMS AND STRENGTHS 4 CONTRAINDICATIONS 5 WARNINGS AND PRECAUTIONS 6 ADVERSE REACTIONS 7 DRUG INTERACTIONS 8 USE IN SPECIFIC POPULATIONS 8.1 Pregnancy 8.2 Labor and Delivery 8.3 Nursing Mothers 8.4 Pediatric Use 8.5 Geriatric Use 9 DRUG ABUSE AND DEPENDENCE 9.1 Controlled Substance 9.2 Abuse 9.3 Dependence 10 OVERDOSAGE 11 DESCRIPTION 12 CLINICAL PHARMACOLOGY 12.1 Mechanism of Action 12.2 Pharmacodynamics 12.3 Pharmacokinetics 12.4 Microbiology (by guidance) 12.5 Pharmacogenomics (by guidance) 13 NONCLINICAL TOXICOLOGY 13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility 13.2 Animal Toxicology and/or Pharmacology 14 CLINICAL STUDIES 15 REFERENCES 16 HOW SUPPLIED/STORAGE AND HANDLING 17 PATIENT COUNSELING INFORMATION NO Comment: Subsections "8.6 Hepatic Impairment" and "8.7 Renal Impairment" were additionally added under "Section 8 Use in Specific Population" according to 21 CFR 201.56(d)(2). 33. The preferred presentation for cross-references in the FPI is the section (not subsection) heading followed by the numerical identifier. The entire cross-reference should be in italics and enclosed within brackets. For example, “[see Warnings and Precautions (5.2)]” or “[see Warnings and Precautions (5.2)]”. SRPI version 3: October 2013 Reference ID: 3604386 Page 7 of 10 Selected Requirements of Prescribing Information N/A Comment: Several references are not italicized 34. If RMCs are listed in HL, the corresponding new or modified text in the FPI sections or subsections must be marked with a vertical line on the left edge. Comment: FULL PRESCRIBING INFORMATION DETAILS FPI Heading YES 35. The following heading must be bolded and appear at the beginning of the FPI: “FULL PRESCRIBING INFORMATION”. This heading should be in UPPER CASE. Comment: N/A BOXED WARNING Section in the FPI 36. In the BW, all text should be bolded. Comment: 37. The BW must have a heading in UPPER CASE, containing the word “WARNING” (even if more than one Warning, the term, “WARNING” and not “WARNINGS” should be used) and other words to identify the subject of the Warning (e.g., “WARNING: SERIOUS INFECTIONS and ACUTE HEPATIC FAILURE”). Comment: YES CONTRAINDICATIONS Section in the FPI 38. If no Contraindications are known, this section must state “None.” Comment: YES ADVERSE REACTIONS Section in the FPI 39. When clinical trials adverse reactions data are included (typically in the “Clinical Trials Experience” subsection of ADVERSE REACTIONS), the following verbatim statement or appropriate modification should precede the presentation of adverse reactions: N/A “Because clinical trials are conducted under widely varying conditions, adverse reaction rates observed in the clinical trials of a drug cannot be directly compared to rates in the clinical trials of another drug and may not reflect the rates observed in practice.” Comment: N/A 40. When postmarketing adverse reaction data are included (typically in the “Postmarketing Experience” subsection of ADVERSE REACTIONS), the following verbatim statement or appropriate modification should precede the presentation of adverse reactions: “The following adverse reactions have been identified during post-approval use of (insert drug name). Because these reactions are reported voluntarily from a population of uncertain size, it is not always possible to reliably estimate their frequency or establish a causal relationship to drug exposure.” Comment: PATIENT COUNSELING INFORMATION Section in the FPI NO SRPI version 3: October 2013 Reference ID: 3604386 Page 8 of 10 Selected Requirements of Prescribing Information NO 41. Must reference any FDA-approved patient labeling in Section 17 (PATIENT COUNSELING INFORMATION section). The reference should appear at the beginning of Section 17 and include the type(s) of FDA-approved patient labeling (e.g., Patient Information, Medication Guide, Instructions for Use). Comment: The reference "See FDA-approved Patient Labeling" should indicate type of FDAapproved patient labeling (i.e., Patient Information). 42. FDA-approved patient labeling (e.g., Medication Guide, Patient Information, or Instructions for Use) must not be included as a subsection under section 17 (PATIENT COUNSELING INFORMATION). All FDA-approved patient labeling must appear at the end of the PI upon approval. Comment: FDA-approved patient labeling must not be included as a subsection under section 17. SRPI version 3: October 2013 Reference ID: 3604386 Page 9 of 10 Selected Requirements of Prescribing Information Appendix A: Format of the Highlights and Table of Contents SRPI version 3: October 2013 Reference ID: 3604386 Page 10 of 10 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------MARY H CHUNG 08/04/2014 Review completed 11/26/2013 Reference ID: 3604386 MEMORANDUM Department of Health and Human Services Food and Drug Administration Center for Drug Evaluation and Research Date: May 30, 2014 To: Donna Griebel, M.D., Director Division of Gastroenterology and Inborn Error Products Through: Michael Klein, Ph.D., Director Silvia Calderon, Ph.D., Team Leader Controlled Substance Staff (CSS) From: Katherine Bonson, Ph.D., Pharmacologist Controlled Substance Staff Subject: Evaluation of Abuse-Related Studies Akynzeo (Netupitant and Palonosetron HCI Fixed-Dose Combination Capsule) (300 mg netupitant + 0.5 mg palonosetron in hard gelatin capsules for oral administration) NDA 205,718 (IND 73,493) Indication: Prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of cancer chemotherapy, including highly emetogenic chemotherapy (HEC) Sponsor: Helsinn Healthcare, SA PDUFA Goal Date: September 26, 2014 Materials reviewed: Abuse-related preclinical and clinical data in NDA submission (eCTD 0000, 9/27/13) Table of Contents 1 BACKGROUND ................................................................................................................... 2 2 CONCLUSIONS .................................................................................................................. 2 3 RECOMMENDATIONS..................................................................................................... 4 4 DISCUSSION ........................................................................................................................ 5 1 of 16 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718 1. Background This memorandum responds to a consult request by the Division of Gastroenterology and Inborn Error Products (DGIEP) to evaluate abuse-related preclinical and clinical data submitted by Helsinn Healthcare in NDA 205,718 for Akynzeo (Netupitant and Palonosetron HCI Fixed-Dose Combination Capsule). This product is a drug combination in a hard gelatin capsule that contains three 100 mg netupitant tablets and one palonosetron 0.50 mg soft gelatin capsule for oral administration. The drug product is indicated for the prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of cancer chemotherapy, including highly emetogenic chemotherapy (HEC). The recommended dose is one capsule administered approximately one hour prior to the start of chemotherapy. Since chemotherapy typically consists of multiple exposures to anti-neoplastic agents over multiple cycles, Akynzeo will be used by patients on a chronic basis. Netupitant is a new molecular entity that is a neurokinin (NK)-1 receptor antagonist. The first-in-class NK-1 antagonist, aprepitant (Emend), was approved in the U.S. in 2006 for the prevention of postoperative nausea and vomiting. The drug label for Emend does not contain Section 9.0 Drug Abuse and Dependence, suggesting there are no abuse-related data available for aprepitant. The NDA for another NK-1 antagonist, casopitant, was withdrawn in 2009 because of concerns regarding cardiovascular toxicity. Palonosetron (Aloxi) is a 5HT3 antagonist that was approved in the U.S. in 2003. Aloxi is marketed in two formulations (0.25 mg, i.v. and 0.5 mg, p.o.) for use in the prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of moderately and highly emetogenic chemotherapy. The drug label for Aloxi does not contain Section 9.0 Drug Abuse and Dependence, suggesting there are no abuse-related data available for palonosetron. There are currently no netupitant + palonosetron drug combinations marketed in any country. However, in January 2014, a Marketing Authorisation Application submitted by Helsinn Healthcare was accepted for review by the European Medicines Agency (EMA) for a combination product containing netupitant + palonosetron. Neither netupitant or palonosetron is a scheduled substance under the Controlled Substances Act (CSA). 2. Conclusions CSS has reviewed the nonclinical and clinical abuse-related data submitted in NDA 205,718 for the netupitant + palonosetron drug combination (Akynzeo) and concludes that this drug combination does not have abuse potential. Notably, many studies were conducted with netupitant alone, since it is a new molecular entity that has not been evaluated previously for abuse potential. The conclusion that netupitant + palonosetron does not have abuse potential is based on the results from the following:  Receptor binding studies show that palonosetron is a high affinity 5HT3 ligand and that netupitant is a high affinity ligand at NK-1 receptors. Netupitant also 2 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718 induces 67% inhibition at the dopamine transporter and 75-100% inhibition at calcium channels, but these data were not converted to Ki values. The abuserelated binding profile for netupitant is incomplete because it did not test the affinity of netupitant for dopamine, glutamate, cannabinoid and 5HT2 receptors. However, an evaluation of the behavioral signs in animal studies conducted with netupitant does not show any abuse-related signals, as described below.  Four toxicology studies with netupitant (with or without palonosetron) were conducted in rats (for 13 and 26 weeks) and beagle dogs (for 13 weeks and 9 months), each with an 8-week recovery period. There were no abuse-related behaviors observed during the drug administration period and no withdrawal-like behaviors observed during the drug discontinuation period.  In a pharmacokinetic/pharmacodynamic study in baboons with netupitant + palonosetron, there were no behavioral effects observed.  In an Irwin study of general behavior with rats, there were no abuse-related behaviors observed following administration of netupitant alone.  In a drug discrimination study with baboons, netupitant + palonosetron did not generalize to either a sedative benzodiazepine (lorazepam or diazepam) or to the stimulant/hallucinogen MDMA. These data suggest that netupitant + palonosetron does not produce activity similar to that of a GABA agonist or an inhibitor of the dopamine/serotonin transporter.  In a self-administration study with baboons, netupitant + palonosetron did not produce levels of self-administration that were different from those produced by vehicle. These data suggest that netupitant + palonosetron does not produce rewarding effects.  In physical dependence studies conducted in rats, beagle dogs and olive baboons, chronic administration of netupitant + palonosetron, or netupitant alone, did not produce withdrawal-like behaviors upon drug discontinuation. This suggests that netupitant (with or without palonosetron) does not produce physical dependence.  In human pharmacokinetic studies, netupitant has a Tmax of 4-5 hours and an elimination half-life of 30-100 hours. Palonosetron has a Tmax of 3-6 hours and an elimination half-life of 40-50 hours.  In humans, 3 major metabolites of netupitant (M1, M2 and M3) are produced, representing 11%, 47% and 16% of the parent drug, respectively. Since there are no abuse-related behavioral signals associated with chronic administration of netupitant alone (or with palonosetron) in humans, the data do not suggest that any of the active metabolites of netupitant have abuse potential. There are no major metabolites of palonosetron. 3 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718  Clinical studies conducted with netupitant + palonosetron in healthy individuals and in cancer patients do not show a pattern of adverse events (AEs) indicative of abuse potential. The most frequently reported central nervous system (CNS)related AE was headache (2.4%). The draft label submitted by the Sponsor does not include Section 9.0 (Drug Abuse and Dependence), based on their conclusion that netupitant + palonosetron does not have abuse potential. Although CSS agrees with this conclusion, based on the data described above, Section 9.0 should be added to the drug label and should accurately reflect the abuse-related study data submitted in the NDA for netupitant + palonosetron. 3. Recommendations  CSS recommends the addition of Section 9.0 (Drug Abuse and Dependence) to the drug label for netupitant + palonosetron, with the following language: Section 9.0 (Drug Abuse and Dependence) 9.1 Controlled Substance Akynzeo (a drug product containing netupitant and palonosetron) is not scheduled under the Controlled Substances Act. 9.2 Abuse The drug combination of netupitant and palonosetron does not produce any signs indicative of abuse potential in preclinical or clinical studies. 9.3 Dependence In physical dependence studies conducted in rats, beagle dogs and olive baboons, chronic administration of netupitant and palonosetron did not produce withdrawal-like behaviors upon drug discontinuation. These data suggest that netupitant and palonosetron does not produce physical dependence.  CSS and CDER should not recommend the netupitant + palonosetron drug combination for control under the CSA, because the results from abuse potential studies show that the drug combination lacks abuse potential. 4 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718 4. Discussion A. Chemistry of Netupitant Netupitant is 2-[3,5-bis(trifluoromethyl)phenyl]-N,2-dimethyl-N-[4-(2-methylphenyl)-6(4-methylpiperazin-1-yl)pyridin-3-yl]propanamide. It is a white to off-white crystalline powder that is freely soluble in toluene and acetone, soluble in isopropanol and ethanol, and very slightly soluble in water. The molecular formula is C30H32F6N4O with a molecular weight of 578.61. Its CAS number is 290297-26-6 Palonosetron HCl is (3aS)-2-[(S)-1-azabicyclo [2.2.2]oct-3-yl]-2,3,3a,4,5,6-hexahydro-1oxo-1Hbenz[de]isoquinoline hydrochloride. It is a white to off-white crystalline powder that is freely soluble in water, soluble in propylene glycol, and slightly soluble in ethanol and 2-propanol. The molecular formula is C19H24N2O.HCl, with a molecular weight of 332.87. Its CAS number is 135729-61-2. B. Pharmacology of Netupitant 1. Receptor Binding Studies (Study #1006030, NETU 10-24, NETU 10-16) Receptor binding studies were conducted with netupitant, since it is a new molecular entity. Binding studies were not conducted with palonosetron, since it was established that palonosetron is a selective 5HT3 antagonist when the drug was first approved by FDA in 2003. Study Design and Results Netupitant was tested at 0.10 and 10 μM for affinity at 50 receptor sites. In these tests, it was shown that netupitant is a high affinity neurokinin (NK) 1 receptor ligand, with a pKi 9.0 (data were not converted to Ki values). Netupitant also has lower affinity for NK2 (pKi 5.8) and NK3 (pKi 7.5) receptors. In addition, netupitant has > 50% inhibition at histamine H2 (95%), adenosine A3 (78%), dopamine transporter (DAT; 67%), L-type Ca2+ channel (75-100%) and muscarinic M1 (52%) sites. The percent inhibition data for these sites were not converted to pKi or Ki values. In contrast to the high affinity that netupitant has for NK receptors, it does not have significant affinity (> 50% inhibition) for other CNS sites, including: opioid (mu, kappa and delta), GABA (GABA-A and GABA-B), acetylcholine nicotinic, serotonin 5HT4, histamine (H1, H3), monoamine transporters (serotonin and norepinephrine), glycine, and the potassium channel. However, it is notable that the Sponsor did not assess netupitant at other CNS sites that are associated with abuse potential, such as dopamine sites, glutamate sites, cannabinoid sites, and serotonin 5HT2 sites. 5 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718 Conclusions Although netupitant has high affinity at NK-1 receptors, it also produces > 50% inhibition at two sites associated with scheduled drugs of abuse (DAT and calcium channels). Since the data for DAT and calcium channel were not converted to pKi or Ki values, it is not clear whether activity at these sites might affect the abuse potential of netupitant. In addition, the lack of information on the affinity of netupitant at other receptors known to be associated with abuse potential (dopamine, glutamate, cannabinoid and 5HT2) makes this receptor binding profile incomplete. 2. Preclinical Behavioral Studies a. Behavioral Observations in Rat and Beagle Dog Toxicology Studies (Study #NETU 07-21, 07-22, 07-19, 07-18) Four toxicology studies were conducted in which animal behavior was monitored following administration of either the combination of netupitant and palonosetron (13 week study in rats and in beagle dogs) or netupitant alone (26 week study in rats and 9 month study in beagle dogs). Each of these studies had an 8 week monitored recovery period. The doses selected were based on evaluating a full toxicological range of doses. These studies show that netupitant (alone or with palonosetron) produces only limited behavioral changes, either during drug administration or following drug discontinuation. 13-Week Rat Study with Netupitant and Palonosetron (with 8 week recovery) Rats (n = 10 males and females/group) were given oral netupitant and palonosetron for 13 weeks, followed by an 8-week recovery period (n = 5 males and females). The dosing groups were as follows: 0 mg/kg (control) 1 mg/kg Netupitant and 2 mg/kg Palonosetron 3 mg/kg Netupitant and 6 mg/kg Palonosetron 10 mg/kg Netupitant and 18 mg/kg Palonosetron 18 mg/kg Palonosetron alone 10 mg/kg Netupitant alone Behavioral observations included: daily clinical signs and weekly evaluation of body weight and food consumption. During the treatment period, increased salivation was noted in a large number of males and females that received the high dose 10 mg/kg netupitant and 18 mg/kg palonosetron dose combination. This may be due to palonosetron, since a comparable incidence of salivation was noted in both sexes that received palonosetron alone. There were no other behavioral observations or changes in body weight or food consumption. 6 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718 During the recovery period there were no behavioral observations or changes in body weight or food consumption. 13-Week Beagle Dog Study with Netupitant and Palonosetron (with 8 week recovery) Beagle dogs (n = 4 males and females/group) were given oral netupitant and palonosetron for 13 weeks, followed by an 8-week recovery period (n = 2 males and females). The dosing groups were as follows: 0 mg/kg (controls) 1 mg/kg Netupitant and 3 mg/kg Palonosetron 3 mg/kg Netupitant and 5 mg/kg Palonosetron 10 mg/kg Netupitant and 10 mg/kg Palonosetron Behavioral observations included: daily clinical signs and weekly evaluation of body weight and food consumption. During the treatment period, salivation (moderate to severe) and shaking of the head were frequently noted in males and females in dogs that received 10 mg/kg netupitant and 10 mg/kg palonosetron. Body weight gain was significantly reduced in females that received 10 mg/kg netupitant and 10 mg/kg palonosetron during Weeks 6-13 of treatment. During recovery, there was a decrease in body weight and body weight gain in females that received 10 mg/kg netupitant and 10 mg/kg palonosetron, but this was observed in the two dogs that were already the smallest ones in the group. There were no other changes in female dogs that received lower doses or in males at the highest dose. 6.5-Month (26-Week) Rat Study with Netupitant Alone (with 8 week recovery) Rats (n = 20 males and females/group) were given oral netupitant alone (1, 3, and 10 mg/kg) for 6.5 months (26 weeks), followed by an 8-week recovery period (n = 10 males and females). Behavioral observations included daily clinical signs and weekly evaluation of body weight and food consumption. During the observation period, there were no clinical signs of toxicity or other behaviors noted. During treatment, there was reduced body weight gain in females treated that received the 10 mg/kg dose started at Week 4. However, in the same female animals, there was reduced food consumption only during the first half of the treatment period. During the recovery period, the body weights of these female animals returned to control values. During the recovery period, there was an increase in food consumption for females. 7 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718 9-Month (36-Week) Beagle Dog Study with Netupitant Alone (with 8 week recovery) Beagle dogs (n = 4/each male and female/group) received oral vehicle, 1, 3 or 10 mg/kg netupitant alone for 9 months, followed by an 8-week recovery period (n = 3/group for vehicle and 10 mg/kg netupitant). Behavioral observations included daily clinical signs and weekly evaluation of body weight and food consumption. During the treatment period, there were no behavioral changes. There was a decrease in body weight gain in males at 10 mg/kg in Weeks 4-5, in females at 10 mg/kg up to Week 6 and in Weeks 17 and 23-27. During the recovery period, there were no changes in behavior or body weight. b. Irwin Screen with Netupitant (Study #1006030) Study Design Male Wistar rats (n = 3/dose) received a single oral dose of netupitant at 100, 300 or 1000 mg/kg prior to observation using the Irwin screen. The animals were observed using a standard Irwin screen protocol at 1, 3 and 6 hours after dosing. Observations included: occurrence of vocalization, stereotypies, aggressiveness, abnormal gait, Straub tail, tremor, twitches, convulsions, body posture, sedation, catalepsy, ptosis, exophthalmos, salivation, lacrimation, piloerection, abnormal respiration, defecation, urination and death; increase or decrease of spontaneous activity, touch response, body tonus and pupil size; increase of sniffing, grooming, scratching and rearing; decreased pinna reflex, traction response and grip strength and any additional observed behaviors. Results There were no unusual behaviors after the 100 mg/kg dose. At 1, 3 and 6 hours following oral administration of netupitant, animals showed difficulty in breathing at 300 mg/kg (2 of 3 animals) and 1000 mg/kg (3 of 3 animals). There was no effect on gait, reflexes or other neurological signs. Body weight and food and water intake were reduced at all dose levels, with body weight being markedly reduced at 24 hour mark following oral administration of the 300 and 1000 mg/kg dose. At the highest dose, one of three rats had trouble breathing and was later found dead. Conclusions There were no abuse-related behavioral observations following administration of netupitant. 8 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718 c. Drug Discrimination Study (Study #NETU 11-25) The drug discrimination study in animals is a pivotal animal behavioral study for abuse potential assessment and is reviewed in detail. The Sponsor conducted two drug discrimination studies in which netupitant was tested either for its ability to generalize to a benzodiazepine (a Schedule IV sedative) or MDMA (a Schedule I stimulant). Study Design This study used olive baboons (N=3) that had been trained to discriminate either a benzodiazepine or MDMA from vehicle. For the benzodiazepine condition, baboons had been previously trained to discriminate 1.8 mg/kg lorazepam p.o. (n = 3) or 1.8 mg/kg diazepam p.o. (n = 1) from vehicle. For the MDMA condition, baboons (n = 3) had been trained to discriminate either 1.8 or 3.2 mg/kg MDMA p.o. from vehicle (n = 2 and n = 1, respectively). The daily 20-min training sessions began 60 minutes after oral dosing with the training drug or vehicle. The fixed ratio (FR) schedule of reinforcement varied between animals, based on the number of responses that best maintained performance of that animal (ranging from FR 20-30). Criterion performance was defined as 95% stimulus-appropriate lever responses in four consecutive training sessions (two each for drug or vehicle). Baboons were tested with vehicle and with the training dose of the training drug to verify drug stimulus control prior to the initiation of test sessions with netupitant + palonosetron. The netupitant + palonosetron doses (mg/kg, p.o.) were, respectively: 3.0/0.005, 8.0/0.013, 10.0/0.020, 13.3/0.025, 18.0/0.030. The Sponsor states that the test doses and testing times were selected based on the results of a pharmacokinetics/pharmacodynamics study. Results In benzodiazepine-trained baboons, all 5 doses levels of netupitant + palonosetron produced responding in all animals that was almost exclusively on the vehicle-associated lever (e.g., <5% on the drug-associated lever). In the MDMA-trained baboons, all 5 doses levels of netupitant+ palonosetron produced responding in two of three animals almost exclusively on the vehicle-associated lever (e.g., <5% on the drug-associated lever). The third animal, however, showed full generalization to MDMA (>80% responding on the MDMA-associated lever) at the highest dose of netupitant + palonosetron (18.0/0.030 mg/kg, respectively). The investigator then re-tested all three baboons at this highest dose and all of the animals responded exclusively on the vehicle lever. Conclusions Netupitant + palonosetron fixed combinations do not share interoceptive stimulus effects with either a benzodiazepine or MDMA. However, it is important to note that drug 9 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718 discrimination is based on the premise that the pharmacological mechanism of action underlies the ability of one drug to generalize to another, based on the interoceptive cues produced by that pharmacological mechanism. Thus, given that netupitant is an NK-1 antagonist and palonosetron is a 5HT3 antagonist, it is unlikely that this drug combination would produce an interoceptive cue similar to that of a GABA agonist (benzodiazepine) or an inhibitor of the dopamine and serotonin transporter (MDMA). Given that there are no known drugs of abuse that are NK-1 antagonists or 5HT3 antagonists, a drug discrimination study such as this one is of little value in assessing the abuse potential of netupitant + palonosetron. d. Self-Administration Study (Study #NETU-11-24) The self-administration study in rats is a pivotal animal behavioral study for abuse potential assessment and is reviewed in detail. The Sponsor conducted a selfadministration drug study in which netupitant was tested for its ability to induce selfadministration as a measure of the rewarding property of the drug. Study Design Male olive baboons (n = 3) were trained to self-administer cocaine (0.32 mg/kg/infusion, i.v.). After stable cocaine self-administration was produced using a fixed ratio (FR) 160 with a 3 hour timeout between injections, animals were allowed access to netupitant + palonosetron (0.20/0.0003, 0.6/0.0010, 1.0/0.0020 mg/kg, i.v.). The Sponsor states that the test doses and testing times were selected based on the results of a pharmacokinetics/ pharmacodynamics study. Results The number of netupitant + palonosetron infusions that were self-administered was similar to that produced by vehicle alone at all doses of the drug combination that were tested. Additionally, there were no behavioral effects observed after the first selfinjection of each dose of the drug combination. Conclusion Netupitant + palonosetron was not self-administered and this drug combination does not appear to have rewarding or reinforcing properties. 3. Physical Dependence Studies in Animals The Sponsor conducted five physical dependence studies with netupitant: two toxicological studies each in rats and beagle dogs, and one dedicated physical dependence study in olive baboons. 10 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718 a Physical Dependence Assessments in Rat and Beagle Dog Toxicology Studies (Study #NETU 07-21, 07-22, 07-19, 07-18) As described above in Section B.2.a (Preclinical Behavioral Studies), four toxicology studies were conducted in which behavior was monitored for 8 weeks after drug discontinuation, following administration of either the combination of palonosetron and netupitant (13 week study in rats and in beagle dogs) or netupitant alone (26 week study in rats and 9 month study in beagle dogs). None of the animals in any of these studies showed any behaviors during the recovery period indicative of physical dependence. Thus, netupitant, either alone or in combination with palonosetron, does not appear to induce physical dependence. b. Physical Dependence Study in Baboons (Study #NETU-11-26) Study Design Male olive baboons (n = 4) received 14 days of vehicle (i.g.) with 15 minutes of behavioral observations per day to establish a baseline, followed by netupitant + palonosetron at 10.0/0.020 mg/kg (i.g.), for 30 days. Since netupitant + palonosetron will be used chronically in cancer patients, the 30-day exposure to these drugs is appropriate for investigating physical dependence. The Sponsor states that the test doses and testing times were selected based on the results of a pharmacokinetics/ pharmacodynamics study. During the first 15 days of netupitant treatment, as well as the last 5 days of treatment, animals were observed daily for 60 minutes after drug administration to evaluate overt behaviors. At the conclusion of the drug administration period, animals received 14 days of vehicle administration, immediately followed by 15 minutes of observation. Under all conditions, the opportunity to respond for food was available 20 hours/day using a FR10 schedule of reinforcement. Following the behavioral observations, animals performed a fine motor coordination task in which an investigator presented a raisin in each of six cups, and the baboon was given 2 minutes to retrieve all of them. The following were recorded: time (seconds) taken to retrieve the treats; whether any treats were dropped; and whether an animal displayed ataxia or other unusual signs. Animals also received a physical examination with ketamine sedation (dose and route not provided) on the following occasions: a) in between the vehicle sessions and the initiation of the netupitant sessions, b) on Day 15 or 16 of netupitant administration, c) on Day 29 or 30 of netupitant administration, d) at the conclusion of the drug discontinuation sessions. A withdrawal score was calculated for each of the first 14 days of drug discontinuation, based on 1 point assigned for each of the 9 behaviors listed below. The behaviors assessed were: 11 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718          Number of pellets consumed in 20 hour decreased Time to complete raisin task increased One or more of the following postures increased: lying down, head lower than torso, withdrawn and/or instances of eyes being closed Locomotion increased or decreased Self-directed behaviors increased (nose rub, nose wipe, scratching, grooming, wet dog shake, masturbation) Aggression increased Tremor, jerk or rigidly braced posture increased Nausea or vomiting increased Seizure occurred If the score contained any one of the following signs, the withdrawal for that day was considered “moderate”: tremor/jerk/rigidly-braced posture, or nausea and vomiting. Occurrence of a seizure would result in characterization as “severe.” All other signs generally were considered indicative of a “mild” withdrawal. Additionally, given the long half-life of the drug combination, alterations in feeding behavior were monitored for a total of 30 days after drug discontinuation, as an indicator of physical dependence. Results A withdrawal score was calculated for each day across the first 14 days of the drug withdrawal period. Animals received a point for each of the nine behaviors observed, but only if the frequency of the behavior was statistically significantly different (using a z score, which conveys information about where a response falls along a normal distribution, in terms of standard deviations from the mean) from baseline and behaviors observed during the end of drug administration period. Out of a maximum possible score of 9, the daily scores for each of the 4 animals ranged from 0-3 across the entire 14 days drug discontinuation period (see below). All behaviors were characterized as “mild”. Individual Baboon Daily Score Range: KR score = 0-1 Day 2 - lying down Day 3 - self-directed (nose rub) MC score = 0-1 Days 5 and 8 - withdrawn posture SK score = 0-1 Day 1 - low pellets Day 7 - high self-directed (grooming); Day 13 - longer to do raisin task 12 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718 WL score 0-3 Day 1 - increased locomotion, aggression (bruxism) self-directed (nose-rub) Day 2 - self-directed (nose-rub) Days 4 and 5 - refused raisin task Days 6 and 9 - longer on raisin task and wet dog shake Day 10 - refused raisin task Day 11 - refused raisin task and There were no changes in feeding behavior in any of the 4 animals over the 30 day drug discontinuation period. This contrasts with the reduction in feeding behavior that was observed during the netupitant + palonosetron administration period. Conclusions There were no behavioral observations during the drug discontinuation period that are suggestive of withdrawal behavior. However, it is notable that netupitant produces three active metabolites in animals and humans (see below, C.1.b and C.2.b), which are detectable from 48 hours (2 days) to 336 hours (14 days) after netupitant administration (see C.2.b below). Since these metabolites have activity as NK-1 antagonists (see C.1.b, below), the metabolites may have contributed to the lack of a withdrawal syndrome in baboons by providing continuing NK-1 receptor blockade. If this is the case, similar conditions are likely to be present in humans, suggesting that there will be a similar lack of a withdrawal syndrome in patients who discontinue netupitant + palonosetron due to metabolite activity. Additionally, the present physical dependence study evaluated behavior for 14 days after netupitant discontinuation, which is the outer limits of the activity of the netupitant metabolites. Thus, if a withdrawal syndrome exists for NK-1 antagonists, it is likely that at least some withdrawal behaviors would have been apparent during this two-week period. The lack of withdrawal behaviors during drug discontinuation suggests that netupitant + palonosetron does not produce physical dependence. Procedurally, it is unclear how exposure to ketamine on three occasions prior to the drug discontinuation period affected behavioral responses during that period. Given the lack of evidence of withdrawal-like behaviors, it is possible that ketamine had no effect. But it is also possible that ketamine, in combination with an NK-1 antagonist and a 5HT3 antagonist, could have suppressed or otherwise altered withdrawal-like behaviors. C. Pharmacokinetics 1. Animal Pharmacokinetics a. Pharmacokinetics and pharmacodynamics of netupitant Baboons (n = 4) were given an oral dose of netupitant + palonosetron (0/0; 3 mg/0.005 mg, 10 mg/0.02 mg, 30 mg/0.05 mg) or vehicle, followed by a 15-min structured 13 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718 observations at 0.5, 1, 2, 4, 6, 8, 24, and 48 hours. Plasma levels of netupitant were dosedependent, with a Tmax at 4 hours and levels remaining high for 8 hours. The Cmax was ~100 ng/ml in all baboons at doses of 10 mg/kg. None of the tested doses of netupitant + palonosetron produced overt behavioral effects in baboons across the 24-hour observation period. This is similar to the results observed in the rat and beagle dog toxicity tests, where no overt behaviors were observed. b. Metabolite profile of netupitant and palonosetron The baboon pharmacokinetic study with netupitant shows that there are 3 active metabolites (>10% of parent): the desmethyl derivative, M1; the N-oxide derivative, M2; the OH-methyl derivative, M3. The three metabolites have activity as NK-1 antagonists, similar to the parent, netupitant. Palonosetron does not produce active metabolites (>10% of parent). This metabolite profile is similar to that observed in humans (see below). 2. Human Pharmacokinetics a. Pharmacokinetics of netupitant In humans, the proposed therapeutic dose of 300 mg oral netupitant is absorbed rapidly (Tmax = 4-5 hours). For the proposed therapeutic dose of 0.5 mg oral palonosetron, the Tmax is 3-6 hours. The elimination half-life of netupitant ranges from 30-100 hours, while the elimination half-life of palonosetron ranges from 40-50 hours. Pharmacokinetic parameters were similar in cancer patients and in healthy volunteers. b. Metabolite profile of netupitant and palonosetron Similar to animals, there are 3 active metabolites of netupitant have been detected in human plasma: M1, M2 and M3 (which have (respectively) 11%, 47% and 16% of the parent). All three metabolites were detectable for long periods after netupitant administration, with the following timeframes: M1 = 176-336 hours, M2 = 48-120 hours, M3 = 144-336 hours. As shown below in Section D (Clinical Studies), there are no abuse-related signals associated with administration of netupitant in humans, so there are no data suggestive that the active metabolites of netupitant produce AEs indicative of abuse potential. In humans, as in animals, palonosetron does not produce any major metabolites (>10% of the parent). 14 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718 D. Clinical Studies The following information was culled from Sponsor summaries of clinical studies submitted in the NDA. A total of 3592 individuals participated in Phase 1, 2 and 3 studies in which netupitant alone or netupitant + palonosetron was administered. Phase 1 studies were conducted in healthy volunteers who were exposed to oral netupitant alone (10 studies) or to oral netupitant in combination with palonosetron (10 studies). The doses of netupitant in Phase 1 studies ranged from 10 to 450 mg. Notably, a human abuse potential study with netupitant + palonosetron was not deemed necessary by CSS during drug development, given that preclinical abuse-related studies (general behavioral studies, self-administration study, and drug discrimination study) showed that this drug combination produced no abuse-related signals. Phase 2/3 studies (a total of 4 studies) tested netupitant at doses of 100, 200 and 300 mg, with netupitant administered alone or in combination with palonosetron. Although all AEs were evaluated during clinical studies with netupitant, Standardized MedDRA Queries (SMQs) were selected a priori to evaluate CNS and psychiatric effects that might reflect abuse-related events. These included euphoric mood, anxiety, insomnia, sleep disorder, and obsessive thoughts, delirium, psychosis, and psychotic disorders. There was only one individual who participated in any of the Phase 1 and Phase 2/3 studies with netupitant + palonosetron who reported a euphoric mood-related AE. In this single incident (1 of 3592, < 0.001%), a healthy individual reported euphoria after receiving 600 mg netupitant + 1.5 mg palonosetron in a pharmacokinetic study with moxifloxacin. Notably, the doses of netupitant and palonosetron administered to this individual were (respectively) two and three times greater than that of the proposed therapeutic doses of 300 mg netupitant and 0.5 mg palonosetron. This isolated case report is not representative of the centrally-mediated responses to netupitant and palonosetron and thus not indicative that this drug combination has abuse potential. With all cycles of Phase 2 (n = 1418) and Phase 3 (n = 1862) studies were combined, there were 533 of the 3280 patients (16.3%) who reported CNS-related AEs, including nervous system disorders (3.3%; 108 of 3280 patients; primarily accountable by headache at 2.4% and dizziness at 2.3%) and psychiatric disorders (3.2%; 106 of 3280 patients; primarily accountable by insomnia at 2.1%). There were no reports of euphoria-related AEs. When the multicycle Phase 3 trials (testing 300 mg netupitant + 0.5 mg palonosetron) were analyzed separately from the combined Phase 2/3 trials, 362 of 1862 patients (19.4%) reported CNS-related AEs of interest. As with the Phase 2/3 population, the AEs of highest frequency were psychiatric disorders (4.8%, primarily accountable by insomnia at 3.3%), and nervous system disorders (4.5%, primarily accountable by headache at 2.4% and dizziness at 3.3%). There were no reports of euphoria-related AEs. 15 Reference ID: 3515856 Netupitant + Palonosetron (Akynzeo) NDA 205,718 Conclusion: In both Phase 1 and Phase 2/3 clinical studies with netupitant, and with netupitant + palonosetron, there were only isolated abuse-related signals and only a single report of euphoria. Thus, there does not appear to be any abuse potential associated with netupitant, or with netupitant + palonosetron, when it is administered to humans. 16 Reference ID: 3515856 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------KATHERINE R BONSON 05/30/2014 SILVIA N CALDERON 05/30/2014 MICHAEL KLEIN 05/30/2014 Reference ID: 3515856 MEMORANDUM DEPARTMENT OF HEALTH AND HUMAN SERVICES PUBLIC HEALTH SERVICE FOOD AND DRUG ADMINISTRATION CENTER FOR DRUG EVALUATION AND RESEARCH ____________________________________________________________________________ DATE: May 29, 2014 TO: Donna Griebel, M.D. Director Division of Gastroenterology and Inborn Error Products (DGIEP) Office of Drug Evaluation III Office of New Drugs FROM: Michael F. Skelly, Ph.D., Pharmacologist Bioequivalence Branch Division of Bioequivalence and GLP Compliance Office of Scientific Investigations THROUGH: Sam H. Haidar, Ph.D., R.Ph. Chief, Bioequivalence Branch Division of Bioequivalence and GLP Compliance Office of Scientific Investigations (OSI) and William H. Taylor, Ph.D. Director Division of Bioequivalence and GLP Compliance Office of Scientific Investigations SUBJECT: Review of EIRs covering NDA 205-718, Akynzeo (Netupitant and Palonosetron HCl combination capsule), sponsored by Helsinn Healthcare At the request of the Division of Gastroenterology and Inborn Error Products (DGIEP), the Division of Bioequivalence and GLP Compliance (DBGLPC) conducted inspections of the clinical and analytical portions of the following bioequivalence study: Study Number: Study Title: Reference ID: 3514940 NETU-09-07 "Bioequivalence study of a new netupitant/ palonosetron fixed combination (300 mg/0.50 mg) versus extemporaneous combination of netupitant 300 mg and palonosetron 0.50 mg after single dose administration to healthy male and female volunteers" Page 2 – NDA 205-718, Akynzeo (Netupitant and Palonosetron HCl combination capsule), sponsored by Helsinn Healthcare The inspection of the clinical portion was conducted by Alexandra B. Pitkin (ORA Investigator, LOS-DO) at Cross Research S.A., in Arzo, Switzerland, from April 28 to May 2, 2014. There were no objectionable findings during the inspection and Form FDA-483 was not issued. The inspection of the analytical (b) (4) portion was conducted by (b) (4) (b) (4) There were no objectionable findings during the inspection and Form FDA-483 was not issued. During the 2008 inspection of study PALO-06-16 for palonosetron NDA 22-233, we raised the possibility of ex vivo reduction of palonosetron N-oxide (M9) back to palonosetron, as discussed in technical publications on other N-oxide drug metabolites, and in drug alone Helsinn's patents on netupitant N-oxide (M2) as a (b) (4) or in combination with palonosetron. Since then, demonstrated that the N-oxide metabolites of palon tron and netupitant are sufficiently stable ex vivo that their reduction back to the parent amine drugs, during storage and handling of plasma samples, does not interfere with measurement of the parent amine drugs in plasma. Conclusion: Following review of the inspectional findings, I recommend that:  The results from the clinical and bioanalytical portions of study NETU-09-07 are acceptable for Agency review. Michael F. Skelly, Ph.D. Bioequivalence Branch, DBGLPC, OSI Final Classifications: Cross Research S.A., Arzo, Switzerland - NAI (FEI# 3008374644) (b) (4) Reference ID: 3514940 - NAI Page 3 – NDA 205-718, Akynzeo (Netupitant and Palonosetron HCl combination capsule), sponsored by Helsinn Healthcare CC: CDER OSI PM TRACK OSI/DBGLPC/Taylor/Dejernett/CF OSI/DBGLPC/BeB/Haidar/Choi/Skelly OSI/DBGLPC/GLPB/Bonapace/Dasgupta CDER/OND/ODEIII/DGIEP/Chung CDER/OND/OCP/Noory ORA/LOS-DO/Pitkin Draft: MFS 5/28/2014 Edits: YMC 5/29/2014; SHH 5/29/2014 OSI: File BE6658; O:\BE\EIRCOVER\205718.hel.NetPal.doc ECMS: Cabinets/CDER_OC/OSI/Division of Bioequivalence & Good Laboratory Practice Compliance/Electronic Archive/BEB FACTS: 8745314 Reference ID: 3514940 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------MICHAEL F SKELLY 05/29/2014 SAM H HAIDAR 05/29/2014 WILLIAM H TAYLOR 05/30/2014 Reference ID: 3514940 Akynzeo (netupitant/palonosetron hydrochloride) Pediatric and Maternal Health Staff Review NDA 205718 Suv'cet.b 0? .1, 0 May 2014 1'70"] Consult Request Date: From: Through: To: Drug: Application Number: Re: Sponsor: Proposed Indication: Proposed Dosage form and Route of administration: *4 {6 DEPARTMENT OF HEALTH HUMAN SERVICES Public Health Service 13~ Food and Drug Administration Of?ce of New Drugs - Immediate Of?ce Pediatric and Maternal Health Staff Silver Spring, MD 20993 Telephone 301-796-2200 FAX 301-796-9744 A October 8, 2013 Erica Radden, MD. Pediatric and Matemal Health Staff, Of?ce of New Drugs Hari Cheryl Sachs, M.D., Team Leader Pediatric and Maternal Health Staff, Of?ce of New Drugs Lynne Yao, OND Associate Director Pediatric and Matemal Health Staff, Of?ce of New Drugs Division of Gastroenterology and Inbom Errors Products (DGIEP) Akynzeo (netupitant/palonosetron NDA 205718 (IND 73,493) Review of the Pediatric Plan Helsinn Healthcare SA For the prevention of acute and delayed nausea and vomiting associated with initial and repeat causes of highly emetogenic cancer chemotherapy and moderately emetogenic cancer chemotherapy. ?xed dose combination capsule of palonosetron 0.5 mg and netupitant 300 mg; oral Proposed Dosing regimen: single oral dose one hour prior to highly and moderately Reference ID: 3510980 emetogenic chemotherapy Page 1 of4 Akynzeo (netupitant/palonosetron hydrochloride) Pediatric and Maternal Health Staff Review NDA 205718 May 2014 Consult Request: DGIEP requests assistance from the Pediatric and Maternal Health Staff (PMHS) in evaluating the sponsor?s Pediatric Plan. Materials Reviewed: - Palonosetron and Netupitant Fixed?Dose Combination Capsule Background Package, (March 15, 2013) - request for a Pediatric Plan for netupitant/palonosetron, NDA 205718 (March 12, 2014) - Sponsor?s response to request (March 12, 2014) for a Pediatric Plan for netupitant/palonosetron, NDA 205718 (March 26, 2013) - Sponsor?s revised Pediatric Plan for netupitant/palonosetron, NDA 205718 (April 4, 2014) - Prior PMHS consult review for netupitant/palonosetron IND 73493 (May 13, 2013) Background: Akynzeo (netupitant/palonosetron hydrochloride) is ?xed dose combination capsule comprised of netupitant, a substance P/neurokinin 1 antagonist, and palonosetron hydrochloride, a serotonin subtype 3 (5-HT3) receptor antagonist. The proposed indication is prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of highly emetogenic cancer chemotherapy and moderately emetogenic cancer chemotherapy. Reviewer comment: Nausea and vomiting associated with initial and repeat courses of cancer cltemotlzerapies will be referred to as CINV. Regulatory Background: The sponsor submitted an NDA for an oral formulation of netupitant/palonosetron ?xed dose combination (FDC) on September 27, 2013. Despite advice at the pre-NDA meeting held on April 16, 2013, that a @(4?would not likely be granted for pediatric studies, the NDA submission contained a request for a The request was based on Although the Division advised the sponsor on March 12, 2014, that a (mo would not be granted and requested submission of a revised Pediatric Plan, the sponsor submitted a letter further reiterating their reasons for requesting a Consequently, a teleconference was held between the sponsor, the Division and PMHS on April 28, 2014, in which the Agency?s position was clari?ed. The sponsor was advised that they would need to attempt to develop an age-appropriate formulation, (which could include formulations other than oral) and submit a pediatric plan detailing the studies they propose to conduct to address PREA along with a tirneline. Accordingly, the sponsor submitted a pediatric plan on April 4, 2014. DGIEP requested assistance with review of the application (see the prior PMHS consult review for netupitant/palonosetron, IND 73493, dated May 13, 2013 reference ID: 3307725], for further regulatory background information). Page 2 of 4 Reference ID: 3510980 Akynzeo (nempitant/palonosetron hydrochloride) Pediatric and Maternal Health Staff Review NDA 205718 May 2014 Sponsor?s Pediatric Plan: The sponsor proposes to conduct three juvenile toxicity studies in rats and dogs: (mo At the same time the sponsor plans to initiate these non-clinical studies, the sponsor plans to begin development of an age-appropriate formulation for studies. To support the initial pediatric clinical study, the sponsor proposes to develop an age-appropriate formulation of netupitant (as a single agent) to be used with palonosetron. The sponsor plans to develop a single-agent oral liquid formulation of netupitant for patients birth to <18 years of age, which would be given with palonosetron1 orally. If the sponsor is rmable to develop an oral liquid netupitant formulation, the sponsor proposes to develop an oral solid netupitant formulation for patients 6 to <17 years of age using age-appropriate dosage based on body weight ranges. An IV formulation of netupitant will be developed for use in combination with the IV formulation of palonosetron for use in patients S6 years of age. W4) If no oral formulation can be developed (liquid or solid) for use in pediatric patients down to 6 years of age, then this proposed mm mm formulation would be used for all pediatric age groups for the initial PIQPD study, and would be administered concomitantly with IV palonosetron via separate IV injections. Use of the (m4) formulation (cmrently under development) in pediatric patients would be contingent upon demonstration of safety and effectiveness in adults in planned adult clinical studies. Based on the contingencies of the development of an age-appropriate formulation for the initial study and outcomes of the pediatric clinical trial, a ?nal (oral or IV) pediatric age-appropriate combination formulation would be developed and used in a pediatric safety and ef?cacy trial. Reviewer comment: I he O?ice of the Chief Counsel was consulted regarding the use of a netupitant mm to address PREA for netupitant/palonosetron. Based on their feedback, if the sponsor cannot develop an age appropriateformulation of the combination of netupitant (and not the netupitant (mm) and palonosetron, then there would be no pediatric formulation of netupitant/palonosetron with which to label any data derived from studies with the netupitant Consequentlv, the development of the could not be compelled under PREA. Additionally, if we agree that the sponsor has made reasonable attempts to develop an age-appropriate combination product of netupitant/palonosetron and is unsuccessful, then a partial waiver may be granted in the age group that is unable to use the existingformulation. In order to obtain the waiver, the sponsor would need to provide data to support this claim for review by the Division and which would be publicly The ?oral? fomiulation of palonosetron that the sponsor proposes to study with netupitant is. in fact. the IV formulation which will be given orally. This is similar to the agreed upon administration of palonosetron in the studies being performed under WR for palonosetron. NDA 21372. Page 3 of 4 Reference ID: 3510980 Akynzeo (netupitant/palonosetron hydrochloride) NDA 205718 Pediatric and Maternal Health Staff Review May 2014 posted. Notably, only one product thus far has qualified for a waiver for this reason (Vimovo [naproxen/esomeprazole magnesium], NDA 22511). A future NDA submission (b) (4) of the any formulation (as a new active ingredient, new dosage form, and potentially new dosage regimen) would trigger PREA, however. The proposed clinical studies consist of: (1) an initial PK/PD pediatric trial of single dose netupitant given concomitantly (in separate formulations) with single dose palonosetron (2) a pediatric clinical efficacy and safety trial of the netupitant/palonosetron FDC compared to standard therapy in pediatric cancer patients 0-17 years of age undergoing treatment with emetogenic chemotherapy. For the safety and efficacy trial, the sponsor plans to conduct either an add-on superiority trial of netupitant/palonosetron FDC compared to palonosetron, or a non-inferiority study of the FDC compared to aprepitant used with a 5HT3 receptor antagonist. The active comparator will be determined based on the standard of care for the treatment of the pediatric cancer population at the time of protocol preparation. Comments on the Pediatric Research Equity Act (PREA) and the Pediatric Plan: Under PREA, all applications for new active ingredients, new indications, new dosage forms, new dosing regimens, or new routes of administration are required to contain an assessment of the safety and effectiveness of the product for the claimed indication(s) in pediatric patients unless this requirement is waived, deferred, or inapplicable. PREA is triggered by this new ingredient. The sponsor proposes to conduct studies in all pediatric (b) (4) age groups However, the sponsor should be advised that if they are unable to develop an age-appropriate formulation of the (b) (4) netupitant/palonosetron combination without the use of a netupitant , they would be eligible for a partial waiver of studies in the pediatric populations for which an ageappropriate formulation could not be developed. Additionally, the non-clinical reviewers have determined that only a single 8-week juvenile toxicity study in rats is required which does not need to be completed prior to the initiation of pediatric clinical trials. Therefore, the sponsor’s proposed studies in nonclinical section should be replaced with this required study. Furthermore, based on these recommended revisions to the pediatric development plan regarding formulation development and nonclinical study requirements, the timeline for the pediatric development plan should be revised accordingly to initiate clinical studies sooner. PMHS reviewed the background materials and provided input on the proposed pediatric plan, in addition to assisting in preparation for the Pediatric Review Committee (PeRC) meeting on May 14, 2014. PMHS participated in the internal meetings from October, 2013 to April, 2014; the PeRC preparation meeting on April 14, 2014; and the sponsor teleconference on March 28, 2014. PMHS also plans to participate in the additional internal meetings scheduled through June, 2014. Our input will be reflected in the approval letter. Page 4 of 4 Reference ID: 3510980 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------ERICA D RADDEN 05/21/2014 HARI C SACHS 05/22/2014 I agree with these recommendations. LYNNE P YAO 05/23/2014 Reference ID: 3510980 VI 5? Cu.? DEPARTMENT OF HEALTH HUMAN SERVICES Public Health Service 0? .1, 1 1?74 in Date: From: Through: To: Drug: NDA: Subject: Applicant: Pediatric and Maternal Health Staff Of?ce of New Drugs Center for Drug Evaluation and Research Food and Drug Administration Silver Spring, MD 20993 Tel 301-796-2200 FAX 301-796-9744 Pediatric and Maternal Health Staff Review May 16, 2014 Consult Date: January 14, 2014 Carrie eresa, Pharm D, MPH Regulatory Reviewer, Maternal Health Team Pediatric and Maternal Health Staff Jeanine Best, MSN, RN, PNP Team Leader, Maternal Health Team Pediatric and Maternal Health Staff Lynne P. Yao, M.D., 0ND Associate Director, Pediatric and Maternal Health Staff The Division of Gastroenterology and Inbom Errors Products (DGIEP) (netupitant/palonosetron) ?xed dose combination capsule 205-7 1 8 Labeling recormnendations for subsections 8.1 and 8.3 Helsinn Healthcare Materials Reviewed: 0 September 26, 2013, Helsinn Healthcare NDA submission 0 Draft DGIEP Pharmacology/Toxicology draft labeling language and review Consult Question: requests Maternal Health Team?s assistance in the labeling review of this application.? Reference ID: 3508235 INTRODUCTION On September 26, 2013, Helsinn Healthcare submitted NDA 205-718 for Netupitant and Palonosetron HCL fixed dose combination capsule for the prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of moderately and highly emetogenic cancer chemotherapy. The proprietary name AKYNZEO® was conditionally accepted for this combination drug product on December 13, 2013. Palonosetron, a serotonin subtype 3 (5HT3) antagonist, was initially approved on July 25, 2003, as an injectable formulation and is marketed as Aloxi® (NDA 21-372). A capsule formulation of Aloxi® (palonosetron) was subsequently approved on August 22, 2008 (NDA 22-233); however, the product was withdrawn from marketing on September 4, 2012, for reasons not related to safety of effectiveness.1 Netupitant is a Neurokinin 1 (NK1) antagonist. DGIEP consulted the Pediatric and Maternal Health Staff – Maternal Health Team (PMHSMHT) to review and update the Pregnancy and Nursing Mothers information in the Akynzeo labeling. This review provides recommended revisions and structuring of existing information related to the Pregnancy and Nursing Mothers labeling in order to provide clinically relevant information for prescribing decisions and to comply with current regulatory requirements. BACKGROUND Palonosetron Palonosetron2 is a 5-HT3 receptor antagonist indicated for:  Moderately emetogenic cancer chemotherapy -- prevention of acute and delayed nausea and vomiting associated with initial and repeat courses  Highly emetogenic cancer chemotherapy -- prevention of acute nausea and vomiting associated with initial and repeat courses  Prevention of postoperative nausea and vomiting (PONV) for up to 24 hours following surgery. Efficacy beyond 24 hours has not been demonstrated Netupitant Netupitant is an NK1 receptor antagonist. Netupitant is being developed for use in combination with palonosetron for the prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of cancer chemotherapy, including highly emetogenic chemotherapy.3 Chemotherapy-induced nausea and vomiting (CINV) Nausea and vomiting is a common side effect associated with the administration of chemotherapeutic drugs. Nausea and vomiting can cause weight changes, dehydration, electrolyte imbalances and fatigue.4 Although nausea and vomiting are related they are also 1 https://www.federalregister.gov/articles/2012/09/04/2012-21652/determination-that-aloxi-palonosetronhydrochloride-capsules-05-milligram-base-were-not-withdrawn 2 Approved package insert for Aloxi®(palonosetron hydrochloride), February 6, 2014. 3 Stathis, M., Pietra, C., Rojas, C., Slusher, B. (2012). Inhibition of substance P-mediated responses in NG108-15 cells by netupitant and palonosetron exhibit synergistic effects. European Journal of Pharmacology, 689, 25-30. 4 Navari, R. (2013). Management of Chemotherapy-Induced Nausea and Vomiting. Drugs, 73:249–262. doi: 10.1007/s40265-013-0019-1 2 Reference ID: 3508235 separate events and often one is treated without the other. Females who experienced severe emesis during pregnancy are believed to be at greater risk for experiencing CINV.5 DISCUSSION Review of Data Pregnancy A search of published literature was performed and no data was found with the use of palonosetron or netupitant in pregnant women. No adverse findings were noted in the animal reproduction studies conducted with palonosetron.6 However, evidence of developmental toxicity (i.e., external and skeletal abnormalities and reduction in fetal weight) was seen in animal reproduction studies in rabbits with netupitant.7 Lactation The Drugs and Lactation Database (LactMed)8 was searched for available lactation data on with the use of palonosetron or netupitant, and no information was located. The LactMed database is a National Library of Medicine (NLM) database with information on drugs and lactation geared toward healthcare practitioners and nursing women. The LactMed database provides any available information on maternal levels in breast milk, infant blood levels, any potential effects in the breastfed infants, if known, as well as alternative drugs that can be considered. The database also includes the American Academy of Pediatrics category indicating the level of compatibility of the drug with breastfeeding. Pregnancy and Nursing Mothers Labeling The Proposed Pregnancy and Lactation Labeling Rule (PLLR) published in May 2008. While still complying with current regulations during the time when the Final Rule is in clearance, PMHS-MHT is structuring the Pregnancy and Nursing mothers label information in the spirit of the Proposed Rule. The first paragraph in the pregnancy subsection of labeling provides a risk summary of available data from outcomes of studies conducted in pregnant women (when available), and outcomes of studies conducted in animals, as well as the required regulatory language for the designated pregnancy category. The paragraphs that follow provide more detailed descriptions of the available human and animal data, and when appropriate, clinical information that may affect patient management. The goal of this restructuring is to provide relevant animal and human data to inform prescribers of the potential risks of the product during pregnancy. Similarly for nursing mothers, human data, when available, are summarized. When only animal data are available, just the presence or absence of drug in milk is noted and presented in nursing mothers labeling, not the amount. Additionally, information on pregnancy testing, contraception, and infertility that has been located in other sections of labeling are now presented in a subsection, Females and Males of Reproductive Potential. 5 Jordan, K., Sippel, C., Schmoll, H-J. (2007). Guidelines for Antiemetic Treatment of Chemotherapy-Induced Nausea and Vomiting: Past, Present and Future Recommendations. The Oncologist, 12:1143-1150. doi: 10.1634/theoncolgoist.12-9-1143. 6 Chopra, Y. pharmacology/toxicology review for Aloxi. 7/11/2003. 7 See DGIEP pharmacology/toxicology review for Akynzeo. 8 United States National Library of Medicine. TOXNET Toxicology Data Network. Drugs and Lactation Database (LactMed). http://toxnet.nlm.nih.gov/cgi-bin/sis/htmlgen?LACT 3 Reference ID: 3508235 CONCLUSION Based on a lack of human pregnancy data and adverse embryo-fetal ?ndings in animals, PMHS recommends that Akynzeo be classi?ed as a Pregnancy Category drug.9 The pregnancy subsection of the labeling was structured in the spirit of the proposed PLLR, while complying with current labeling regulations. PMHS-MHT deleted the sponsor?s probpgsed The labeling regulations allow omission of inapplicable subsections (see 21 FR 201 Any relevant Akynzeo would have been placed in subsection 8.1 Pregnancy in proposed PLLR format. The nursing mothers subsection of labeling was revised to comply with current labeling recommendations. PMHS-MHT discussed our labeling recormnendations with DGIEP at a meeting on April 24, 2014. PMHS-MHT and the DGIEP Pharmacology/Toxicology team recormnendations are below and re?ect the discussions with DGIEP at that meeting. PMHS-MHT refers to the NDA action for ?nal labeling. The sponsors draft labeling recommendation can be formd in Appendix A. LABELING RECOMMENDATIONS 8 USE IN SPECIFIC POPULATIONS 8. 1 . Pregnancy Pregnancy Category Risk Summary Adequate and well-controlled studies with AKYNZEO have not been conducted in pregnant women. In animal reproduction studies, no effects on embryo-fetal development were observed following dail administration of netupitant in pregnant rats during the period of organogenesis at doses up to times the human AUC at the recommended single human dose to be given with each cycle of chemotherapy. However, a dose-dependent increase in adverse effects on embryo- fetal development was observed following daily administration of netupitant in pregnant rabbits dm?ing the period of organogenesis with doses at least mmtimes the hlunan AUC at the recommended single human dose to be given with each cycle of chemotherapy. Daily administration of netupitant in rats up to (5m) times the hmnan AUC at the recommended human dose dtu?ing organogenesis through lactation produced no adverse effects in the In animal reproduction studies with palonosetron, no effects on embryo-fetal development were observed following oral administration during the period of organogenesis at doses 11p to 921 and 1841 times the recommended hmnan oral dose in rats and rabbits, respectively. AKYNZEO should be used during pregnancy only if the potential bene?t justi?es the potential risk to the fetus. 9 Pregnancy Category De?nition: Animal reproduction studies have shown an adverse effect on the fetus. there are no adequate and well controlled studies in humans. AND the bene?ts from the use of the drug in pregnant women may be acceptable despite its potential risks. OR animal studies have not been conducted and there are no adequate and well controlled studies in humans. Reference ID: 3508235 Animal Data (b) (4) Daily administration of up to 30 mg/kg netupitant in rats ( times the human AUC at the recommended single human dose to be given with each cycle of chemotherapy) during the period of organogenesis produced no effects on embryo-fetal development. However, an increased incidence of external and skeletal abnormalities in rabbit fetuses was observed following daily (b) (4) administration of netupitant in rabbits at 10 mg/kg/day and higher times the human AUC at the recommended single human dose to be given with each cycle of chemotherapy) during the period of organogenesis. These abnormalities included positional abnormalities in the limbs and paws, and fused sternebrae. Reduction in fetal rabbit weight occurred at 30 mg/kg/day. Maternal toxicity in rabbits (i.e. loss of bodyweight during the treatment period) was also (b) (4) observed at 30 mg/kg/day. Daily administration of up to 30 mg/kg netupitant times the human AUC at the recommended human dose) in rats during organogenesis through lactation produced no adverse effects in the offspring. In animal reproduction studies with palonosetron, no effects on embryo-fetal development were observed in pregnant rats given oral doses up to 60 mg/kg/day (921 times the recommended human oral dose based on body surface area) or pregnant rabbits given oral doses up to 60 mg/kg/day (1841 times the recommended human oral dose based on body surface area) during the period of organogenesis. 8.3 Nursing Mothers It is not known whether AKYNZEO is present in human milk. Because many drugs are present in human milk and because of the potential for tumorgenicity shown for palonosetron in the rat carcinogenicity study [see Non-Clinical Toxicology (13.1)], a decision should be made whether to discontinue nursing or to discontinue the drug, taking into account the importance of the drug to the mother. Appendix A Sponsors Recommendations 8 USE IN SPECIFIC POPULATIONS 8.1 Pregnancy (b) (4) (b) (4) 8.3 Nursing Mothers It is not known whether palonosetron and netupitant, the two components of AKYNZEO, are excreted in human milk. Because many drugs are excreted in human milk and because of the (b) (4) potential for tumorgenicity 5 Reference ID: 3508235 shown for palonosetron in the rat carcinogenicity study, a decision should be made whether to discontinue nursing or to discontinue the drug, taking into account the importance of the drug to the mother. APPEARS THIS WAY ON ORIGINAL 6 Reference ID: 3508235 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------CARRIE M CERESA 05/16/2014 JEANINE A BEST 05/16/2014 LYNNE P YAO 05/21/2014 Reference ID: 3508235 MEMORANDUM DEPARTMENT OF HEALTH AND HUMAN SERVICES PUBLIC HEALTH SERVICE FOOD AND DRUG ADMINISTRATION CENTER FOR DRUG EVALUATION AND RESEARCH ____________________________________________________________________________ CLINICAL INSPECTION SUMMARY DATE: May 12, 2014 TO: Mary Chung, Pharm.D., Regulatory Project Manager Nancy Snow, M.D., Medical Officer Division of Gastroenterology and Inborn Errors Products FROM: Susan Leibenhaut, M.D. Medical Officer Good Clinical Practice Assessment Branch Division of Good Clinical Practice Compliance Office of Scientific Investigations THROUGH: Susan D. Thompson, M.D. Team Leader Good Clinical Practice Assessment Branch Division of Good Clinical Practice Compliance Office of Scientific Investigations THROUGH: Kassa Ayalew, M.D., M.P.H. Acting Branch Chief Good Clinical Practice Assessment Branch Division of Good Clinical Practice Compliance Office of Scientific Investigations SUBJECT: Evaluation of Clinical Inspections NDA: 205718 APPLICANT: Helsinn Healthcare SA DRUG: Akynzeo ® (Netupitant Palonosetron Fixed Dose Combination) NME: Yes THERAPEUTIC CLASSIFICATION: Standard INDICATION: Prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of moderately emetogenic cancer chemotherapy (MEC) and highly emetogenic cancer chemotherapy (HEC) Reference ID: 3505592 Page 2 NDA 205718 Clinical Inspection Summary Product: Akynzeo ® (Netupitant Palonosetron Fixed Dose Combination) Sponsor: Helsinn Healthcare SA CONSULTATION REQUEST DATE: INSPECTION SUMMARY GOAL DATE: DIVISION ACTION GOAL DATE: PDUFA DATE: November 8, 2013 May 16, 2014 September 16, 2014 September 16, 2014 I. BACKGROUND: The sponsor, Helsinn Healthcare SA, submitted this NDA for the netupitant and palonosetron HCI Fixed-Dose Combination Capsule (FDC) for the prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of moderately and highly emetogenic cancer chemotherapy (MEC and HEC). Netupitant is a novel selective NK1 receptor antagonist. Palonosetron is a selective 5-HT3 receptor antagonist that was approved in the US in 2003 in a formulation for intravenous use and in 2008 in an oral formulation. Netupitant is a new molecular entity. The sponsor submitted the following four studies in support of the application: 1. NETU-07-07 entitled “A Randomized, Double-Blind, Parallel Group, Dose-Ranging, Multicenter Study Assessing the Effect of Different Doses of Netupitant or Placebo Administered with Palonosetron and Dexamethasone on the Prevention of Highly Emetogenic Chemotherapy-Induced Nausea and Vomiting in Cancer Patients” 2. NETU-08-18 entitled “A phase III multicenter, randomized, double-blind, double-dummy, active-controlled, parallel group study of the efficacy and safety of oral netupitant administered in combination with palonosetron and dexamethasone compared to oral palonosetron and dexamethasone for the prevention of nausea and vomiting in cancer patients receiving moderately emetogenic chemotherapy” 3. NETU-10-29 entitled “A phase III, multicenter, randomized, double-blind, unbalanced (3:1) active control study to assess the safety and describe the efficacy of netupitant and palonosetron for the prevention of chemotherapy-induced nausea and vomiting in repeated chemotherapy cycles” 4. Palo-10-01 entitled “Single-dose, multicenter, randomized, double-blind, double-dummy, parallel group study to assess the efficacy and safety of oral palonosetron 0.50 mg compared to I.V. palonosetron 0.25 mg administered with dexamethasone for the prevention of chemotherapy-induced nausea and vomiting in cancer patients receiving highly emetogenic cisplatin-based chemotherapy” Reference ID: 3505592 Page 3 NDA 205718 Clinical Inspection Summary Product: Akynzeo ® (Netupitant Palonosetron Fixed Dose Combination) Sponsor: Helsinn Healthcare SA Protocol NETU-07-07 was a multicenter, randomized, active-controlled trial with four principal arms comparing three different doses of oral netupitant combined with oral palonosetron and oral dexamethasone against oral palonosetron and oral dexamethasone (control group). An additional arm with aprepitant administered with ondansetron and dexamethasone was included for exploratory purposes only. The primary efficacy endpoint was the complete response rate (CR) defined as no emetic episodes and no rescue medication, within 120 hours after the start of the highly emetogenic chemotherapy administration. The study was conducted as a Phase 2 study from February 2008 to November 2008 at 44 sites in the Ukraine and Russia and enrolled a total of 694 subjects. According to the clinical study report submitted by the sponsor, the percent of patients with complete response over 0-120 hours after start of cisplatin administration was 76.5% in the palonosetron alone group and 87.4%, 87.6%, and 89.6% in the netupitant 100 mg, 200 mg, and 300 mg groups, respectively. Differences from palonosetron alone were greater than 10% (10.9% to 13.2%). All doses of netupitant were statistically superior to palonosetron alone (p≤0.018). This was designed and conducted as a Phase 2 study. In a meeting on June 18, 2010, the division agreed that NETU07-07 would be acceptable as the lone trial to support the fixed dose combination capsule for the prevention of acute and delayed HEC-CINV, provided review of the data support efficacy and safety. Protocol NETU-08-18 was a Phase III, multicenter, multinational, randomized, double-blind, double-dummy, parallel group, stratified study. It was designed to assess both acute and delayed MEC. The primary evaluation was the proportion of patients with CR (defined as no emesis, no rescue medication) in the delayed phase (time interval 25-120 hours after the start of the MEC administration) at cycle 1. The study was conducted between April 2011 and November 2012 at 177 study centers in 15 countries and enrolled a total of 1455 subjects. Efficacy evaluations were based on the patients’ documentation of emetic episodes (episodes of retching or vomiting) and nausea assessed by Visual Analogue Scale (VAS) and intake of rescue medication. To collect these data, patient diary covering Days 1 to 5 at each cycle were used. According to the conclusion of the study results contained in the clinical study report submitted by the sponsor to the NDA, this study demonstrated the superiority of the netupitant/palonosetron (300 mg/0.50 mg) FDC over palonosetron alone with respect to the primary, CR in the delayed phase, and both key secondary, CR in the acute and overall phases after the administration of moderately emetogenic chemotherapy during the first chemotherapy cycle. Protocol NETU-10-29 was a multicenter, multinational, randomized, active-controlled, doubleblind, double-dummy, unbalanced (3:1), parallel group, stratified study. It was designed to assess the safety and tolerability of a single oral dose of a Fixed-Dose Combination of netupitant and palonosetron (300 mg/0.50 mg) in initial and repeated cycles of chemotherapy. The primary efficacy evaluation was the proportion of patients with CR (defined as no emesis, no rescue medication) in the delayed phase (time interval 25-120 hours after the start of the MEC administration) at cycle 1. It was conducted from July 2011 to September 2012 at 72 centers in 10 countries and randomized 413 subjects. According to the conclusion of the study Reference ID: 3505592 Page 4 NDA 205718 Clinical Inspection Summary Product: Akynzeo ® (Netupitant Palonosetron Fixed Dose Combination) Sponsor: Helsinn Healthcare SA results contained in the clinical study report submitted by the sponsor to the NDA, the netupitant/palonosetron FDC combined with dexamethasone demonstrated high response rates in the prevention of nausea and vomiting, in the delayed, acute and overall phases of initial and repeated cycles of chemotherapy. Protocol Palo-10-01 was a multicenter, multinational, randomized, active-controlled, doubleblind, double-dummy study and was designed to demonstrate the non-inferiority of single dose oral palonosetron 0.50 mg versus single dose Intravenous (I.V.) palonosetron 0.25 mg in terms of percentage of patients with Complete Response (CR) during the acute phase (0-24 hours). The primary efficacy evaluation was the proportion of patients with CR (defined as no emesis, no rescue medication) within 24 hours after the start of HEC administration on Day 1. It was conducted from June 2011 to November 2012 at 80 study sites in 12 countries and enrolled a total of 743 subjects. According to the sponsor, this study demonstrated the non-inferiority of oral palonosetron 0.50 mg compared with I.V. palonosetron 0.25 mg in terms of the primary efficacy endpoint i.e. CR in the acute phase. The review division chose sites for inspection on the basis of several factors including attempt to provide coverage for all four studies, high enrollment, inspectional history of the clinical investigator, geographical diversity and feasibility. In December 2013, when it was not possible to inspect sites in the Ukraine, two sites in India were chosen for NETU0 8-18 and NETU 10-29. Because NETU 07-07 was conducted in Ukraine and Russia only, and inspections in Russia presented difficulties with scheduling and ultimately were not feasible to inspect, it was not possible to provide more than the original Russian site inspection chosen for NETU 07-07. A sponsor inspection was conducted as per usual OSI procedures because this is a new molecular entity. In addition, the sponsor inspection evaluated noncompliance at a Russian site noted in the clinical study report for NETU 07-07 and information concerning monitoring at Ukrainian sites that could not be inspected. Reference ID: 3505592 Page 5 NDA 205718 Clinical Inspection Summary Product: Akynzeo ® (Netupitant Palonosetron Fixed Dose Combination) Sponsor: Helsinn Healthcare SA II. RESULTS (by Site): Name, Address and Type of Inspected Entity Protocol # Site # Inspection and # of Subjects Date Final Classification* CI: Dr. Tibor Csoszi Tószegi út 21, H-5004 Szolnok Hungary NETU-08-18/ Site 5403/ 47 Subjects VAI PALO-10-01/ Site 5405/ 45 Subjects NETU-10-29/ Site 5607/ 30 Subjects PALO-10-01/ Site 5602/ 37 subjects NETU-07-07/ Site 101/ 37 subjects NETU-08-18/ Site 3102/ 55 Subjects January 13 to 23, 2014 CI: Dr. Anna Lowczak January 27 NAI ul. Kuracyjna 30 to 30, 2014 82-550 Prabuty, Poland CI: Dr. Katarzna Zajad January 20 VAI ul. Roentgena 5 02-781 Warszawa, Poland to 24, 2014 Phone: +48.225.462.169 CI: Dr. Anna V. Alyasova December VAI 2 Nizhne-Volzhskaya Nab. 9 to13, 603001 Nizhny Novgorod, Russia 2013 CI: Dr. Mamillapalli Gopichand February NAI #33-25-33 Venkatakrishanayya Street 10 to 14, Suryaraopet 2014 Vijayawada 520002, India CI: Professor Narendra Khippal NETU-10-29/ February 3 NAI S.M.S. College and Hospital Site 4205/ to 7, 2014 Shastri Nagar, Jaipur, India, 302016 20 Subjects Sponsor: NETU-07-07 March 24 Pending* Helsinn Healthcare SA NETU-08-18 to April 4, (preliminary Via Pian Scairolo 9 NETU-10-29 2014 NAI) Pazzallo-Lugano PALO-10-01 Switzerland Key to Classifications NAI = No deviation from regulations. VAI = Deviation(s) from regulations. OAI = Significant deviations from regulations. *Pending = Preliminary classification based on information in 483 or preliminary communication with the field; EIR has not been received from the field, and complete review of EIR is pending. Reference ID: 3505592 Page 6 NDA 205718 Clinical Inspection Summary Product: Akynzeo ® (Netupitant Palonosetron Fixed Dose Combination) Sponsor: Helsinn Healthcare SA 1. Dr. Tibor Csoszi, Szolnok, Hungary a. What was inspected: At this site, for Protocol NETU-08-18, a total of 53 subjects were screened; 47 subjects were enrolled and randomized. For Protocol Palo-10-10, a total of 48 subjects were screened; 45 subjects were enrolled and randomized. Informed consent was verified for all subjects. For Protocol NETU-08-18, an audit of 24 subjects’ records was conducted. The review included subject diaries, ECGs, source records, and test article handling and accountability. For Protocol Palo-10-10 an audit of records from 10 subjects who received study drug (oral palonosetron) was conducted and the remaining 35 subjects’ records (intravenous and oral treatment arms) were reviewed for diary data, chemotherapy administration, and concomitant medications data. b. General Observations/Commentary: For both studies, there was no evidence of under-reporting of adverse events and the efficacy data were verifiable. A Form FDA 483 was issued because, for Protocol Palo-10-10, concomitant medications were not recorded in the eCRF as follows: 1. The concomitant medication Mannisol was not recorded for Subjects 04, 10, 15, 16, 17, 18, 19, 22, 23, 26, 29, 30, 31, 33, 34, 37, 38, 39, 40, 42, 43, 45, 46, 47, and 48. 2. The concomitant medication Suprastin (chloropyramine) was not recorded for Subjects 12, 20, 21, 35 and 48. These violations involved minor record keeping issues and should not affect study outcome. The clinical investigator responded in a letter dated February 3, 2014, promising corrective action. c. Assessment of data integrity: The studies appear to have been conducted adequately, and the data generated by this site may be used in support of the respective indication. 2. Dr. Anna Lowczak, Prabuty, Poland a. What was inspected: At this site, for Protocol NETU-10-29, a total of 31 subjects were screened, 30 subjects were enrolled and 22 subjects completed the study. There was one death. The field investigator reviewed study related documents for 12 subjects. Records reviewed consisted of source documents, eCRFs and medical records. The review also included informed consent documents, inclusion/exclusion criteria, clinical laboratory values, efficacy parameters, study drug accountability, and adverse events. b. General observations/commentary: For the efficacy endpoint data, vomiting, nausea, and rescue medications, there were no discrepancies between the source data and the line listings from the NDA submission provided to the field investigator. There were no discrepancies in the timing of administration of chemotherapy relative to administration of study drug and concomitant Reference ID: 3505592 Page 7 NDA 205718 Clinical Inspection Summary Product: Akynzeo ® (Netupitant Palonosetron Fixed Dose Combination) Sponsor: Helsinn Healthcare SA medications. There was no evidence of under-reporting of adverse events. c. Assessment of data integrity: The study appears to have been conducted adequately, and the data generated by this site appear acceptable in support of the indication. 3. Dr. Katarzna Zajad, Warszawa, Poland a. What was inspected: At this site, for Protocol Palo-10-10, a total of 43 subjects were screened; 37 subjects were enrolled and 33 subjects completed the study. An audit of 16 subjects’ records was conducted. The review included consent form documents, study correspondence, source records, and test article handling and accountability. b. General observations/commentary: A Form FDA 483 was issued because: 1. The investigation was not conducted in accordance with the investigational plan because two adverse events were not reported. Specifically, fatigue was not reported for Subject 560209 (palonosetron IV arm) and anemia during hospitalization was not reported for Subject 560210 (palonosetron IV arm). 2. Failure to maintain adequate case histories: The patient diary for Subject 560231 (palonosetron IV arm) was not available during the inspection. According to the hospital records the subject returned the diaries and data were transcribed into the CRF, however, at the close of the study, the diary was noted to be missing and this was documented in a note to file dated December 10, 2013. The CI could not offer an explanation, but the study team was re-trained by the CI to apply increased attention to prevent the loss of source documentation in the future. Other than Item #1, there was no evidence of under-reporting of adverse events. Except for the isolated Item #2 noted above, the efficacy data were verifiable. Also noted at this site was the fact that the rescue medication log for this study did not include all rescue medication that was dispensed during the study and rescue medications were not returned by the patient. Reviewer Note: Although rescue medication was to be documented in the eCRF, there was no requirement for separate rescue medication accountability logs and the investigator was authorized to use an alternative rescue medication. c. Assessment of data integrity: The violations noted on the Form FDA 483 are considered minor and do not impact data reliability. The study appears to have been conducted adequately, and the data generated by this site appear acceptable in support of the respective indications. Reference ID: 3505592 Page 8 NDA 205718 Clinical Inspection Summary Product: Akynzeo ® (Netupitant Palonosetron Fixed Dose Combination) Sponsor: Helsinn Healthcare SA 4. Dr. Anna V. Alyasova, Novgorod, Russia a. What was inspected: At this site, for Protocol NETU-07-07, a total of 51 subjects were screened; 37 subjects were enrolled and 37 subjects completed the study. The review included consent form documents, study correspondence, source records, and test article handling and accountability. An audit of all enrolled subjects’ records was conducted for consent form document review and endpoint data verification by diary review. b. General observations/commentary: The FDA investigator reviewed 50% of enrolled subjects and found no evidence of under-reporting of AEs. The primary endpoint data were verified in 100% of enrolled subjects. Also it was verified that, in 100% of enrolled subjects, the time of drug administration was within the allowed time window (60 min+2 min) and that the time was recorded accurately in Listing 11, “Study Drug Administration—All Randomized Subjects”. A Form FDA 483 was issued for failure to maintain adequate case histories. Specifically, in 3 of 26 subject diaries reviewed, a data entry error was detected in the corresponding case report form (CRF). The subject diaries for Subjects 101-1082, 101-1481, 101-1396 recorded dexamethasone tablets taken as 1 (Day 2, PM); 1 (Day 3, AM); and 3 (Day 3, AM). The corresponding CRF recorded 2 tables in each case. Each of these subjects drug accountability log reported “0” tablets returned. The discrepancies were not recorded in the protocol deviation log and were not mentioned in the monitoring visits follow-up letters. Dr. Alyasova responded that the errors were in the subject diaries and not in the drug accountability, but that these errors were not detected at the time of entry into the CRFs. She promised corrective action in that more attention will be paid in training subjects to complete diaries and training study staff to be careful about the documentation. c. Assessment of data integrity: The violations noted on the Form FDA 483 are considered minor and do not impact data reliability. The study appears to have been conducted adequately, and the data generated by this site appear acceptable in support of the respective indications. 5. Dr. Mamillapalli Gopichand, Vijayawada 520002, India a. What was inspected: At this site, for Protocol NETU-08-18, a total of 62 subjects were screened, and 55 subjects were enrolled. Records reviewed consisted of source documents, eCRFs, and medical records. The review also included informed consent documents, inclusion/exclusion criteria, clinical laboratory values, study diaries, study drug accountability, and adverse events. The FDA field investigator reviewed 100% of subjects’ records for informed consent documents and primary efficacy endpoint. Reference ID: 3505592 Page 9 NDA 205718 Clinical Inspection Summary Product: Akynzeo ® (Netupitant Palonosetron Fixed Dose Combination) Sponsor: Helsinn Healthcare SA b. General observations/commentary: There was no evidence of under-reporting of adverse events, and the source data for the primary efficacy data were able to be verified at the site. No significant regulatory violations were noted, and no Form FDA 483 was issued. c. Assessment of data integrity: The study appears to have been conducted adequately, and the data generated by this site appear acceptable in support of the respective indications. 6. Professor Narendra Khippal, Jaipur, India, 302016 a. What was inspected: At this site, for Protocol NETU 10-29, a total of 23 subjects were screened, and 20 subjects were enrolled. The field investigator reviewed the informed consent documents and subject diaries for efficacy endpoints for all 20 subjects. A review was conducted of 6 subjects’ records for adverse events and for 13 subjects’ records for eligibility criteria. The review also included study drug accountability. b. General observations/commentary: For the efficacy endpoint data, vomiting, and rescue medications, there were no discrepancies between the source data and the line listings from the NDA submission provided to the field investigator. There was no evidence of under-reporting of adverse events. No regulatory violations were noted and no Form FDA 483 was issued. There were three discussion items. Dr. Khippal failed to document his discussions with the monitor regarding the clarification of SAEs; and failed to document reasons for administration of antibiotics and the impact of potential infections on study participation; He submitted a progress report to the Ethics Committee late. Specifically, he submitted the first progress report to the Ethics Committee on July 11, 2012, instead of in March 2012 when it was due. Dr. Khippal responded verbally to each of the discussion items during the closeout of the inspection. c. Assessment of data integrity: The study appears to have been conducted adequately, and the data generated by this site appear acceptable in support of the respective indications. Reference ID: 3505592 Page 10 NDA 205718 Clinical Inspection Summary Product: Akynzeo ® (Netupitant Palonosetron Fixed Dose Combination) Sponsor: Helsinn Healthcare SA 7. Helsinn Healthcare SA, Pazzallo-Lugano, Switzerland Note: Observations below for the sponsor inspection are based on a draft Establishment Inspection Report (EIR) and e-mail communications with the FDA field investigator. An inspection summary addendum will be issued if conclusions change upon review of the final EIR. a. What was inspected: This inspection evaluated compliance with sponsor responsibilities including selection and oversight of contract research organizations, monitoring, financial disclosure, FDA form 1572s, and quality assurance (QA). A review of the Trial Master Files was conducted. Special attention was requested for the following Ukrainian sites that were chosen for inspection but could not be inspected: Dr. Bondarenko, Site 4207 for Protocol NETU-08-18 and Site 4205 for Protocol NETU-10-29; and Dr. Dudnichenko, Site 213 for Protocol NETU-07-07. In addition, coverage of Dr. Popov, Site 120 for Protocol NETU-07-07 was requested because the sponsor noted in the clinical study report that there were “multiple major audit findings, ranging from failure to meet eligibility criteria and administration of prohibited medications to inconsistencies between source data and CRFs.” These were noted after the study was closed. The number of monitoring files reviewed by the FDA investigator, per study:  NETU-07-07 – Site 210 (Dr. Popov), Site 213 (Dr. Dudnichenko) and 2 additional sites, Site 215 and Site 105 (paper files only for this trial)  NETU-08-18 – Dr. Bondarenko (electronic records)  NETU-10-29 - Dr. Bondarenko plus 3 others randomly chosen (electronic records)  PALO-10-01 - 2 randomly chosen sites reviewed in detail (electronic records) b. General observations/commentary: The sponsor delegated complete responsibility to a CRO for each of these four trials. The CRO selection process was found to be more robust currently and for the latter 3 studies then it was for the initial NETU-07-07 study (initiated in 2007). Concerning the conduct and oversight of NETU-07-07, the Phase II study was initiated in 2007, and was “upgraded” to a pivotal study to be included in the NDA after discussions with FDA in 2010. While the study was ongoing, issues that arose and were noted at Site 120 in Weekly Activities reports included items such as ECGs were not transmitting by phone in some areas, the timing of ECGs and vital signs, the drug supply had repeated issues related to temperatures during transport, and the analog scale in the NCR pages was problematic in that there was a shift of values between the white and pink NCR pages. Reference ID: 3505592 Page 11 NDA 205718 Clinical Inspection Summary Product: Akynzeo ® (Netupitant Palonosetron Fixed Dose Combination) Sponsor: Helsinn Healthcare SA Due to the change in study classification (Phase 2 to Phase 3) and the intent to include it in the NDA submission, the sponsor conducted 13 additional QA audits post-study at 12 sites in 2011 in addition to the original 8 site audits conducted in 2008 and 2009. Site 120 underwent 2 post study audits for data verification and re-verification. At Site 120, the more critical issues revealed during the audits included 21 eligibility issues and the 27 subjects that were found to have unreported adverse events or concomitant medications. The eligibility issues were primarily medication related, i.e. having taken an antiemetic within 24 hours or taken dexamethasone within 4 weeks, but there were also 2 subjects who exhibited some exclusionary criteria in their ECG. Many notes were created by Dr. Popov to explain the issues, but many simply stated that the item was an oversight and not intentional. However, study data could not be added or changed because the database had already been locked by this time. Financial disclosure documents were reviewed extensively and only minor checking or dating issues were found with a very small number of these. c. Assessment of data integrity: There was no evidence through the monitoring reports and QA audits performed to indicate non-compliant PIs (other than Site 120 for Study NETU 07-07) or any under-reporting of AEs. It appears that the issues noted at Site 120 for Study NETU 07-07 were an isolated occurrence and that, other than this instance, the Helsinn oversight of the CROs involved with the 4 studies appeared adequate. The studies appear to have been conducted adequately, and the data generated by these studies appear acceptable in support of the respective indications. III. OVERALL ASSESSMENT OF FINDINGS AND RECOMMENDATIONS Six clinical investigator sites and the sponsor were inspected for this NDA. Coverage of two clinical sites per protocol was achieved with the exception of NETU 07-07. All clinical sites had the classification of NAI or VAI with minor regulatory violations cited. For the sponsor inspection, inspection of monitoring reports provided insight into good clinical practice (GCP) issues noted by the sponsor at Site 120 for Study NETU 07-07. The draft inspection report noted that the issues with Site 120 for Study NETU 07-07 were isolated and related to the unique development plan for this FDC drug. The studies appear to have been conducted adequately, and the data generated by these studies appear acceptable in support of the respective indications. Note: Observations above for the sponsor inspection are based on a draft EIR and e-mail communications with the FDA field investigator. An inspection summary addendum will be issued if conclusions change upon review of the final EIR. Reference ID: 3505592 Page 12 NDA 205718 Clinical Inspection Summary Product: Akynzeo ® (Netupitant Palonosetron Fixed Dose Combination) Sponsor: Helsinn Healthcare SA {See appended electronic signature page} Susan Leibenhaut, M.D. Medical Reviewer Good Clinical Practice Assessment Branch Division of Good Clinical Practice Compliance Office of Scientific Investigations CONCURRENCE: {See appended electronic signature page} Susan D. Thompson, M.D. Team Leader Good Clinical Practice Assessment Branch Division of Good Clinical Practice Compliance Office of Scientific Investigations CONCURRENCE: {See appended electronic signature page} Kassa Ayalew, M.D., M.P.H. Acting Branch Chief Good Clinical Practice Assessment Branch Division of Good Clinical Practice Compliance Office of Scientific Investigations Reference ID: 3505592 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------SUSAN LEIBENHAUT 05/13/2014 SUSAN D THOMPSON 05/14/2014 KASSA AYALEW 05/14/2014 Reference ID: 3505592 Department of Health and Human Services Public Health Service Food and Drug Administration Center for Drug Evaluation and Research Office of Medical Policy PATIENT LABELING REVIEW Date: May 12, 2014 To: Donna Griebel, MD Director Division of Gastroenterology and Inborn Error Products (DGIEP) Through: LaShawn Griffiths, MSHS-PH, BSN, RN Associate Director for Patient Labeling Division of Medical Policy Programs (DMPP) Barbara Fuller, RN, MSN, CWOCN Team Leader, Patient Labeling Division of Medical Policy Programs (DMPP) From: Nathan Caulk, MS, BSN, RN Patient Labeling Reviewer Division of Medical Policy Programs (DMPP) Meeta Patel, Pharm.D. Regulatory Review Officer Office of Prescription Drug Promotion (OPDP) Subject: Review of Patient Labeling: Patient Package Insert (PPI) Drug Name (established name): AKYNZEO (netupitant and palonosetron) Dosage Form and Route: capsules Application Type/Number: NDA 205-718 Applicant: Helsinn Healthcare SA Reference ID: 3505046 1 INTRODUCTION On September 27, 2013, Helsinn Healthcare SA submitted for the Agency’s review an original New Drug Application (NDA) 205-718 for AKYNZEO (netupitant and palonosetron) capsules. The proposed indications for AKYNZEO (netupitant and palonosetron) capsules are for: • • prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of highly emetogenic cancer chemotherapy. prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of moderately emetogenic cancer chemotherapy. This collaborative review is written by the Division of Medical Policy Programs (DMPP) and the Office of Prescription Drug Promotion (OPDP) in response to a request by the Division of Gastroenterology and Inborn Error Products (DGIEP) on October 10, 2013 and October 24, 2014, respectively, for DMPP and OPDP to review the Applicant’s proposed Patient Package Insert (PPI) for AKYNZEO (netupitant and palonosetron) capsules. DMPP conferred with the Division of Medication Error, Prevention, and Analysis (DMEPA) and a separate DMEPA review of the proposed container label, carton labeling and Full Prescribing Information was completed on January 19, 2014. 2 3 MATERIAL REVIEWED • Draft AKYNZEO (netupitant and palonosetron) PPI capsules received on September 27, 2013, revised by the Review Division throughout the review cycle, and received by DMPP on April 25, 2014. • Draft AKYNZEO (netupitant and palonosetron) capsules Prescribing Information (PI) received on September 27, 2013, revised by the Review Division throughout the review cycle, and received by DMPP on April 25, 2014. • Approved EMEND (aprepitant) capsules comparator labeling dated March 20, 2013. • Draft ALOXI (palonosetron HCl) comparator labeling dated April 25, 2014. • Draft AKYNZEO (netupitant and palonosetron) Instructions for Opening dated April 25, 2014. REVIEW METHODS To enhance patient comprehension, materials should be written at a 6th to 8th grade reading level, and have a reading ease score of at least 60%. A reading ease score of 60% corresponds to an 8th grade reading level. In our review of the PPI the target reading level is at or below an 8th grade level. Additionally, in 2008 the American Society of Consultant Pharmacists Foundation (ASCP) in collaboration with the American Foundation for the Blind (AFB) Reference ID: 3505046 published Guidelines for Prescription Labeling and Consumer Medication Information for People with Vision Loss. The ASCP and AFB recommended using fonts such as Verdana, Arial or APHont to make medical information more accessible for patients with vision loss. We have reformatted the PPI document using the Verdana font, size 10. In our collaborative review of the PPI we have: 4 • simplified wording and clarified concepts where possible • ensured that the PPI is consistent with the Prescribing Information (PI) • removed unnecessary or redundant information • ensured that the PPI is free of promotional language or suggested revisions to ensure that it is free of promotional language • ensured that the PPI meets the criteria as specified in FDA’s Guidance for Useful Written Consumer Medication Information (published July 2006) • ensured that the PPI is consistent with the approved comparator labeling where applicable CONCLUSIONS The PPI is acceptable with our recommended changes. 5 RECOMMENDATIONS • Please send these comments to the Applicant and copy DMPP and OPDP on the correspondence. • Our collaborative review of the PPI is appended to this memorandum. Consult DMPP and OPDP regarding any additional revisions made to the PI to determine if corresponding revisions need to be made to the PPI. Please let us know if you have any questions. 5 Page(s) of Draft Labeling have been Withheld in Full as b4 (CCI/TS) immediately following this page Reference ID: 3505046 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------NATHAN P CAULK 05/12/2014 MEETA N PATEL 05/13/2014 BARBARA A FULLER 05/13/2014 LASHAWN M GRIFFITHS 05/13/2014 Reference ID: 3505046 FOOD AND DRUG ADMINISTRATION Center for Drug Evaluation and Research Office of Prescription Drug Promotion Memorandum **PRE-DECISIONAL AGENCY MEMO** Date: May 6, 2014 To: Mary Chung, Pharm D Regulatory Health Project Manager Division of Gastroenterology and Inborn Errors Products From: Meeta Patel, PharmD Regulatory Review Officer Office of Prescription Drug Promotion (OPDP) Subject: NDA 205718 OPDP Comments for draft Akynzeo (netupitant and palonosetron) capsules for oral use PI and PPI OPDP has reviewed the proposed draft PI for Akynzeo (netupitant and palonosetron) capsules for oral use. We have reviewed the draft PI, sent to us on April 25, 2014, and have the following comments. Comments on the draft PPI will be sent under separate cover as a joint review with DMPP. Thank you for the opportunity to comment on the proposed PI. If you have any questions or concerns, please contact Meeta Patel at 301-796-4284 or meeta.patel@fda.hhs.gov. 20 Page(s) of Draft Labeling have been Withheld in Full as b4 (CCI/TS) immediately following this page Reference ID: 3501579 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------MEETA N PATEL 05/06/2014 Reference ID: 3501579 STUDY ENDPOINT CONSULT REVIEW Template version: November 8, 2013 SEALD TRACKING NUMBER IND/NDA/BLA NUMBER LETTER DATE/SUBMISSION NUMBER PDUFA GOAL DATE DATE OF CONSULT REQUEST REVIEW DIVISION MEDICAL REVIEWER REVIEW DIVISION PM SEALD REVIEWER(S) ACTING SEALD ENDPOINTS TEAM LEADER ACTING SEALD DIRECTOR REVIEW COMPLETION DATE DRUG NAME SPONSOR/APPLICANT CLINICAL OUTCOME ASSESSMENT TYPE ENDPOINT(S) CONCEPT(S) MEASURE(S) SPONSOR’S TARGETED INDICATION 2013-174 NDA 205718 09/25/2013 09/26/2014 11/19/2013 Division of Gastroenterology and Inborn Errors Products Nancy Snow/Ruyi He Mary Chung Paivi Miskala Elektra Papadopoulos Sandy Kweder 04/24/2014 Akynzeo™ (netupitant and palonosetron) capsules, for oral use Helsinn Healthcare PRO Nausea Average nausea visual analog scale Prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of highly emetogenic cancer chemotherapy Prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of moderately emetogenic cancer chemotherapy Reference ID: 3495561 SEALD Review Paivi H. Miskala, PhD NDA 205718 A. EXECUTIVE SUMMARY This Study Endpoints and Labeling Development (SEALD) review is provided as a response to a request for consultation by the Division of Gastroenterology and Inborn Errors Products (DGIEP) regarding NDA 205718 for Akynzeo™ (netupitant and palonosetron capsules, for oral use). Based on information provided by the sponsor, the sponsor is targeting an indication for the prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of highly and moderately emetogenic cancer chemotherapy. DGIEP consulted SEALD regarding the Functional Living Index-Emesis (FLIE) (see SEALD review signed off in Darrts 03/04/2014). Following discussion of the FLIE instrument during a labeling meeting on March 12, 2014, DGIEP requested a second SEALD consult regarding sponsor’s nausea assessment. Given the short turnaround for the second SEALD consult, this review was abbreviated to summarize the key issues. Sponsor assessed average nausea severity in the past 24 hours using a 100mm visual analog scale where 0 indicates “no nausea” and 100 indicates “nausea as bad as it could be”. This assessment is used as part of combination endpoints and as stand-alone endpoints in sponsor’s trials. Regulatory history under IND 73493 suggests that there is documented agreement between DGIEP and the sponsor on some of the key trial endpoints in some of the trials. SEALD defers determination of key secondary endpoints (i.e., adequacy of multiplicity adjustment in the (b) (4) statistical analysis plan) to the statistical reviewer. Sponsor proposes to Key issues regarding the nausea assessment are as follows: a) Non-key endpoints which were not included in the multiplicity adjustment of the (b) (4) statistical analysis plan do not provide conclusive evidence of treatment benefit b) Sponsor’s instrument measures average nausea severity, not worst nausea severity in the past 24 hours. This could be problematic since the sponsor is defining “no nausea” as maximum nausea severity < 5 mm as measured on the VAS and “no significant nausea” as maximum nausea severity < 25 mm (maximum refers to maximum average severity of nausea recorded within the time interval to be analyzed, i.e., within overall phase 0-120 hours, acute phase 0-24 hours, delayed phase 25-120 hours,). With average nausea measurement there is no guarantee that maximum average nausea severity was <5 mm in any given day because we are measuring an average, not the worst experience patient had with nausea. For example, it is possible that a patient had nausea > 5mm part of the day, but could have an average nausea measurement of <5 for the day. There is a similar issue with “no significant nausea” cutpoint of < 25 mm using average nausea measurement; it is possible that a patient had significant nausea at some point during the day, but could end up with an average < 25 mm for the day. This would be less problematic if the sponsor had measured worst nausea severity because we would have had some certainty that the nausea was never worse that the cutpoint values during the past 24 hours. Sponsor was requested a copy of the instrument and any empiric evidence to support 2 Reference ID: 3495561 SEALD Review Paivi H. Miskala, NDA 205 718 these cutpoints sponsor responded by sending a copy of the nausea instrument (see appendix of this review) and by referring to the previous labeling for EMEND, but did not provide any additional empiric evidence or justi?cation to support the nausea cutpoints. Thus, there continues to be some rmcertainty whether any claims regarding ?no nausea? or ?no signi?cant nausea? would be misleading based on the prespeci?ed cutpoints given the average nausea measurement. If the sponsor had used the score of 0 as a de?nition of ?no nausea? then that would have been a more appropriate defmition because if the average for the day is 0 then the maximum for the day would likely be 0 as well. DGIEP could consider further evaluation of the sponsor?s trial data to look at distribution of nausea scores for patients who had a nausea score 5mm; what percentage of these patients in each treatment arm have a score of 0? c) Nausea endpoints cannot be interpreted without information on rescue medication use to ensure that any improvement in nausea is not due to rescue medication use similarly to how pain endpoints are evaluated). (1) In general, using a 100 mm Visual analog scale is acceptable, but one should keep in mind that a visual analog scale may give a false sense of precision because it is questionable that patients can a) differentiate 101-levels in severity and b) can visually accurately draw a line without error using these 101-levels, yet we are measru?ing the patient responses with a 100 ruler. e) Submission did not include information if any validation or translation/cultm?al adaptation work was done for the nausea assessment. This review concludes that if any of the nausea endpoints were key endpoints in a phase 3 trial and there is a prior agreement with the FDA on key endpoints then SEALD recommends conservative evaluation of those endpoints to support treatment bene?t claims, given the limitations above, to ensure that there is convincing evidence of treatment bene?t. The sponsor is adequately measuring average nausea severity based on the instrument, although this was not ideal in this particular context. The most challenging limitation is lack of evidence to support the cutpoints chosen for ?no nausea? and ?no signi?cant nausea? given the average nausea . . . . 4 measurement. Also, rescue medrcatron use must be consrdered when evaluatmg nausea. SEALD defers evaluation of the effect of handling of missing values to DGIEP and Of?ce of Biometrics. SEALD defers evaluation of treatment ef?cacy to DGIEP and Of?ce of Biometrics. Reference ID: 3495561 SEALD Review Paivi H. Miskala, NBA 2057 8 B. APPENDICES Reference ID: 3495561 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------PAIVI H MISKALA 04/24/2014 ELEKTRA J PAPADOPOULOS 04/24/2014 Reference ID: 3495561 STUDY ENDPOINT CONSULT REVIEW Template version: November 8, 2013 SEALD TRACKING NUMBER IND/NDA/BLA NUMBER LETTER DATE/SUBMISSION NUMBER PDUFA GOAL DATE DATE OF CONSULT REQUEST REVIEW DIVISION MEDICAL REVIEWER REVIEW DIVISION PM SEALD REVIEWER(S) ACTING SEALD ENDPOINTS TEAM LEADER ACTING SEALD DIRECTOR REVIEW COMPLETION DATE DRUG NAME SPONSOR/APPLICANT CLINICAL OUTCOME ASSESSMENT TYPE ENDPOINT(S) CONCEPT(S) MEASURE(S) INDICATION 2013-174 NDA 205718 09/25/2013 09/26/2014 11/19/2013 Division of Gastroenterology and Inborn Errors Products Nancy Snow/Ruyi He Mary Chung Paivi Miskala Elektra Papadopoulos Sandy Kweder 03/04/2014 Akynzeo™ (netupitant and palonosetron) capsules, for oral use Helsinn Healthcare PRO Impact of nausea and vomiting on daily life Functional living index – emesis (FLIE) Prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of highly emetogenic cancer chemotherapy Prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of moderately emetogenic cancer chemotherapy Reference ID: 3464831 SEALD Review Paivi H. Miskala, NDA 205 718 A. EXECUTIVE SUMMARY This Study Endpoints and Labeling Development (SEALD) review is provided as a response to a request for consultation by the Division of Gastroenterology and Inborn Errors Products (DGIEP) regarding NDA 205718. The sponsor has investigated ef?cacy and safety of oral netupitant administered in combination with palonosetron and dexamethasone compared to oral palonosetron and dexamethasone for prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of highly and moderately emetogenic cancer chemotherapy. DGIEP is consulting SEALD regarding sponsor?s proposal to include claims related to M4) FLIE was not a key trial endpoint in the sponsor?s phase 3 trials. The consult concludes that 09(4) Non-key endpoints, including FLIE, will be considered exploratory evidence, Furthermore, the sponsor did not submit any information to support development and validation content validity, validation, translation and cultru?al adaption) of the FLIE. At face value it is questionable whether patients can determine independent contributions of nausea and vomiting on their daily life when both of these are present (see section 3 for additional review ?ndings regarding FLIE item content). For these reasons SEALD will not be requesting additional information from the sponsor (SEALD does not review development and validation of exploratory endpoints) unless DGIEP is considering (hm) B. COMNIENTS TO Not applicable. Reference ID: 3464831 SEALD Review Paivi H. Miskala, PhD NDA 205718 C. STUDY ENDPOINT REVIEW *** Information related to FLIE was collected in one of the sponsor’s two phase 3 trials (NETU08-18 included FLIE, NETU-10-29 did not include FLIE). For that reason the remainder of this review will focus on NETU-08-18. *** 1 CONTEXT OF USE (COU) 1.1 Target Study Population and Clinical Setting Cancer patients receiving moderately emetogenic chemotherapy. 1.2 Clinical Trial Design NETU-08-18 was a phase III multicenter/multinational (177 study sites in 15 countries), randomized, double-blind, double-dummy, active-controlled, parallel group study stratified (by region (United States, Latin America including Mexico, Europe, Commonwealth of Independent States (i.e, former Soviet Republics) and Asia) and age (<55 years and ≥ 55 years). The study was designed to evaluate the efficacy and safety of oral netupitant administered in combination with palonosetron and dexamethasone compared to oral palonosetron and dexamethasone for the prevention of nausea and vomiting in cancer patients receiving moderately emetogenic chemotherapy. Sponsor included the following diagram outlining NETU-08-18 clinical trial design: 3 Reference ID: 3464831 SEALD Review Paivi H. Miskala, PhD NDA 205718 1.3 Endpoint Positioning Sponsor outlined the following endpoints in their NETU-08-18 phase 3 trial: 4 Reference ID: 3464831 SEALD Review Paivi H. Miskala, PhD NDA 205718 Reviewer’s comments: FLIE instrument was not specified as a key study endpoint. Non-key (b) (4) endpoints will be considered exploratory in nature. 5 Reference ID: 3464831 SEALD Review PaiVi H. Miskala, NDA 205 71 8 Table 3: Study 1l'isits and Assessments Cycle Extension Screening Day to ?1 Dayl Day 2?1 Day 5" Day 11{ Visit 1 Visit 2 1?i'isit 3 Visit 4 Visit 5 Informed consent (de Inclusion-"exclusion criteria Demography (de Medical history and ECOG performance status Urine pregnancy test (Xjk Prior and concomitant medications Physical examination Vital signs'E lE?lead itg 3?:g itg LVEF 00d '1th Cardiac Troponin and Blood chemistry Hematology Urinalysis Randomization {Xja Chemotherapy Study drugs and additional studyr drug administration Patient diary and instructions Completed from Day 1 to Day 5? on completion collected at Visit 4 ELIE questionnaire (de Adverse events Pharmacokinetics orApproximately 24 hours after the first study drug administration on Day 1. 120 hours after the first study drug administration holiday or a weekend day Visit 4 was to be scheduled 1within the 2 forthcoming days. Day 21:2, ether on-site or phone contact. If following chemotherapy cycle was scheduled 21 day a?er Day 1 of previous cycle, the follow-up visit and the screening visit of 2 consequent cycles ma; have coincided. Only at cycle 1. Vital signs included pulse rate, systolic blood pressure. and diastolic blood pressure at Visit 1. pre-dose. 5 hours, 24 hours. and 120 hours after the first study drug administration on Day 1 of each cycle: height was measured only at Visit 1 of cycle 1. weight at Visit 1 and Visit 4 of each cycle. 12?lead ECG (single recording) was assessed in a central laboratory. 12?lead ECG was recorded at screening. pre?dose. 5 hours, 24 hours. and 120 hours after the ?rst stud; drug administration on Day 1 of each cycle. End of study only. Adverse events were collected from Informed rConsent to 21 days after Day 1 of last cycle. During cycle 1, in a subgroup of patients. blood samples at pre-specified time schedules for PK. Performed for females of childbearing potential within 24 hours prior to the first study er1_ administration on Day 1 of each cycle. Abbreviations: ECG=Electrocardiogram: ECUG=Eastern Cooperative Oncology Group: FLIE=Fimctiona Living Index-Emesis: Ventricular Ejection Fraction: PK=Pharmac okinetics. Reference ID: 3464831 SEALD Review Paivi H. Miskala, NDA 2057 8 1.4 Labeling or promotional claim(s) based on the COA Sponsor is proposing the following draft labeling language regarding - Reviewer ?s comments: Furthermore, the sponsor submission did not include any information related to development and validation of this instrument to determine whether the instrument measures what it is intended to measure. At face value the instrument is problematic; see section 3 below. 2 CONCEPT OF INTEREST (C01) AND CONCEPTUAL FRAMEWORK Conceptual framework was not included in the submission. Sponsor states that the instrument measures the impact of nausea and vomiting on daily life. See section 3 below for the content of the instrument domains. 3 CLINICAL OUTCOME ASSESSMENT (COA) Functional Living Index-Emesis Sponsor states that the FLIE measures the impact of nausea and vomiting on patients? quality of life. FLIE has 18 questions divided into 2 domains: a) Nausea (questions 1-9): Q1: How much nausea have you had in the past 5 days? Reference ID: 3464831 SEALD Review Paivi H. Miskala, PhD NDA 205718 Q2: Has nausea affected your ability to maintain usual recreation or leisure activities in the past 5 days? Q3: Has nausea affected your ability to make a meal or do minor household repairs during the past 5 days? Q4: How much has nausea affected your ability to enjoy a meal in the past 5 days? Q5: How much has nausea affected your ability to enjoy drinking liquids in the past 5 days? Q6: How much has nausea affected your willingness to see and spend time with family and friends, in the past 5 days? Q7: Has nausea affected your daily functioning in the past 5 days? Q8: Rate the degree to which your nausea has imposed a hardship on you (personally) in the past 5 days? Q9: Rate the degree to which your nausea has imposed a hardship on those closest to you in the past 5 days? b) Vomiting (questions 10-18): Q10: How much vomiting have you had in the past 5 days? Q11: Has vomiting affected your ability to maintain usual recreation or leisure activities during the past 5 days? Q12: Has vomiting affected your ability to make a meal or do minor household repairs during the past 5 days? Q13: How much has vomiting affected your ability to enjoy a meal in the past 5 days? Q14: How much has vomiting affected your ability to enjoy drinking liquids in the past 5 days? Q15: How much has vomiting affected your willingness to see and spend time with family and friends, in the past 5 days? Q16: Has vomiting affected your daily functioning in the past 5 days? Q17: Rate the degree to which your vomiting has imposed a hardship on you (personally) in the past 5 days? Q18: Rate the degree to which your vomiting has imposed a hardship on those closest to you in the past 5 days? Sponsor states that each question is answered using a 100mm (1-7 points) visual analogue scale with anchors corresponding to “none”/”not at all” and “a great deal”. Sponsor outlines in their submission that the instrument is scored as follows: 8 Reference ID: 3464831 SEALD Review Paivi H. Miskala, PhD NDA 205718 Sponsor provided the following formula for calculation of the nausea and vomiting domain scores: Instrument domain scores range from 9 to 63. FLIE total score is the sum of the nausea and vomiting domain scores. The instrument uses 5-day recall period. Reviewer’s comments: At face value this instrument is problematic for the following reasons:  It is questionable whether patients can determine independent contributions of nausea and vomiting on their functioning in daily life if both of these symptoms occur.  The domain scores combine symptom severity (Q1, Q10) with impact of having each symptom to their daily life; therefore, the measurement concept is unclear.  Q9 and Q18 ask about hardship to others which is not a relevant concept to measure when evaluating treatment benefit to the person himself/herself.  Rationale for creating “FLIE points” scores is unclear. Sponsor did not provide a copy of the instrument in their submission. The case report form that was included in the submission did not show the visual analog scales as presented to the patient. No evidence to support instrument development and validation (i.e., content validity, psychometric validation, and translation and cultural adaptation evidence) was included in the submission. 9 Reference ID: 3464831 SEALD Review Paivi H. Miskala, PhD NDA 205718 4 CONTENT VALIDITY Content validity information was not included in the submission. Also, SEALD does not review development and validation of exploratory endpoints. 5 OTHER MEASUREMENT PROPERTIES (RELIABILITY, CONSTRUCT VALIDITY, ABILITY TO DETECT CHANGE) Information related to other measurement properties was not included in the submission. 6 INTERPRETATION OF SCORES Information was not included in the submission. 7 LANGUAGE TRANSLATION AND CULTURAL ADAPTATION Information was not included in the submission. 8 REVIEW USER MANUAL User manual was not included in the submission. 10 Reference ID: 3464831 SEALD Review Paivi H. Miskala, PhD NDA 205718 D. APPENDICES APPEARS THIS WAY ON ORIGINAL 11 Reference ID: 3464831 SEALD Review Paivi H. Miskala, PhD NDA 205718 COPYRIGHT MATERIAL WITHHELD 12 Reference ID: 3464831 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------PAIVI H MISKALA 03/04/2014 ELEKTRA J PAPADOPOULOS 03/04/2014 Reference ID: 3464831 DEPARTMENT OF HEALTH AND HUMAN SERVICES PUBLIC HEALTH SERVICE FOOD AND DRUG ADMINISTRATION CENTER FOR DRUG EVALUATION AND RESEARCH DIVISION OF CARDIOVASCULAR AND RENAL PRODUCTS Date: March 3, 2014 From: CDER DCRP QT Interdisciplinary Review Team Through: Norman Stockbridge, M.D., Ph.D. Division Director Division of Cardiovascular and Renal Products /CDER To: Mary Chung, RPM DGEIP Subject: QT-IRT Consult to NDA 205718 Note: Any text in the review with a light background should be inferred as copied from the sponsor’s document. This memo responds to your consult to us dated Nov 20, 2013 regarding the sponsor’s response to our previous request for ECG data at 15 and 30 minutes. The QT-IRT received and reviewed the following materials:  Your consult  IRT previous review (1/20/2010)  Draft Label Reference ID: 3463762 QT-IRT Comments for DGEIP The sponsor’s response to the QT-IRT’s previous request is acceptable. PROPOSED LABEL SPONSOR’S PROPOSED LABEL 12.2 Pharmacodynamics Cardiac Electrophysiology (b) (4) QT-IRT’S PROPOSED LABEL QT-IRT’s proposed labeling language is a suggestion only. We defer final labeling decisions to the Division. 12.2 Pharmacodynamics Cardiac Electrophysiology (b) (4) BACKGROUND We have previously reviewed the QT study report for this application when it was submitted under IND 73493. In our review we stated that “No significant QTcF prolongation effect of netupitant/palonosetron (therapeutic dose 200 mg/0.50 mg and supratherapeutic dose 600 mg/1.50 mg) was detected in this TQT study (Figure 1).” However, we made the following comment to be conveyed to the sponsor: “The moxifloxacin profile is not exactly what we expected. The rising phase is missing. The maximum moxifloxacin induced ddQTcF effect appears almost at the first available time point, which is 1 hr after dose. We want to understand what happened before hour 1. Please extract data for moxifloxacin, placebo at 15b minute, 30 minute post-dose and the corresponding baseline for us to evaluate.” 2 Reference ID: 3463762 Figure 1: LS Mean and 90% CI ΔΔQTcF Timecourse Source: IRT previous review (1/20/2010), Page 24. The sponsor responded to the above request during the current NDA submission as the following: Due to the timing of the start and end of the 24 hour recordings, there were no data at the Day-1 equivalent of 15 and 30 minutes post dose, since the ECG Holter recording start time was not done on Day -1 with respect to the time of dosing on Day 1. Thus, extractions could only be taken at 35 minutes and 45 minutes post dose on Day 1 of moxifloxacin dosing that corresponded to the equivalent times on Day -1. These data show that there was an increase in QTc at 35 minutes and at 45 minutes similar to the 1 hour time point; hence not showing the expected rise in the moxifloxacin result profile (see Table below). 3 Reference ID: 3463762 Placebo-Corrected Change from Baseline - Estimates fro. Mixed Model mm are Pridericia (mec) Additional Exploratory Analysis to Investigate Early Moxifloxacin OTC Effects Moxifloxacin 400 ng Kati-ate Upper Lower Tile Bound Bound 1112.5- 15 9 11Moxi?oxacin can show an increase in duration after 30 minutes from dosing and the critical time point to determine rise is the 15 minute time point which due to study condition from several years ago was not recorded. While assay sensitivity is shown statistically the clinical pro?le of moxi?oxacin from 0-60 minutes could not be ascertained. Since the pharmacodynamic-kjnetic model showed absolutely no hint of any effect of the study agents on cardiac repolarization the integrity of the results of the trial should not be seriously questioned. Since however the ECG data and the pharmacokinetic-dynamic modelling were completely void of any signal of an effect on cardiac repolarization for this trial, the integrity of the results should not be seriously questioned. Reviewer ?5 comments: Acceptable. The relationships between AAQTCF and drug concentrations were independently investigated in our previous review and no evident exposure-response relationships were observed. Thank you for requesting our input into the development of this product under NDA 205718. We welcome more discussion with you now and in the future. Please feel free to contact us via email at gov Reference ID: 3463762 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------JIANG LIU 03/03/2014 NORMAN L STOCKBRIDGE 03/03/2014 Reference ID: 3463762 Department of Health and Human Services Public Health Service Food and Drug Administration Center for Drug Evaluation and Research Office of Surveillance and Epidemiology Office of Medication Error Prevention and Risk Management Label, Labeling and Packaging Review Date: January 17, 2014 Reviewer: Terri Wood-Cummings, MD Division of Medication Error Prevention and Analysis Team Leader: Lubna Merchant, M.S., Pharm.D Division of Medication Error Prevention and Analysis Drug Name and Strength: Akynzeo (Netupitant and Palonosetron) Capsules 300 mg/0.5 mg Application Type/Number: NDA 205718 Applicant/sponsor: Helsinn Healthcare SA OSE RCM #: 2013-2266 *** This document contains proprietary and confidential information that should not be released to the public.*** Reference ID: 3438270 Contents 1 INTRODUCTION ....................................................................................................... 1 1.1 Regulatory History ............................................................................................... 1 1.2 2 Product Information……………………………………………………………..1 METHODS AND MATERIALS REVIEWED .......................................................... 1 2.1 2.2 Previously Completed Reviews………………………………………………...2 Labels and Labeling ............................................................................................. 1 3 MEDICATION ERROR RISK ASSESSMENT ......................................................... 2 4 CONCLUSIONS………………………………………………………………….....2 4 RECOMMENDATIONS AND COMMENTS ........................................................... 2 Appendices .......................................................................................................................... 4 Reference ID: 3438270 1 INTRODUCTION This review responds to a consult from the Division of Gastroenterology and Inborn Errors Products (DGIEP) to evaluate the proposed container label, carton labeling, and Full Prescribing Information for Akynzeo (NDA 205718) for areas of vulnerability that could lead to medication errors. DGIEP requested this review as part of their evaluation for NDA 205718. PRODUCT INFORMATION 1.1 The following product information is provided in the Applicant’s September 27, 2013 submission: • Active Ingredients: Netupitant and Palonosetron • Indication of Use: Prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of highly emetogenic cancer chemotherapy; prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of moderately emetogenic cancer chemotherapy. • Route of Administration: Oral • Dosage Form: Capsules • Strength: 300 mg/0.5 mg • Dose and Frequency: One capsule orally one hour prior to the start of chemotherapy. • How Supplied: Blister pack of one capsule. • Storage: Store at 20ºC - 25ºC (68ºF - 77ºF); excursions permitted to 15ºC - 30ºC (59º - 86ºF). • Container and Closure System: Product is supplied in an foil blister pack, one capsule per blister pack card. The blister card is packaged in (b) (4) secondary, (Burgopak) packaging. (b) (4) 2 METHODS AND MATERIALS REVIEWED 2.1 LABELS AND LABELING Using the principles of human factors and Failure Mode and Effects Analysis, 1 the Division of Medication Error Prevention and Analysis (DMEPA) evaluated the following: 1 • Container Labels submitted September 27, 2013 (Appendix A) • Carton Labeling submitted September 27, 2013 (Appendix B) Institute for Healthcare Improvement (IHI). Failure Modes and Effects Analysis. Boston. IHI:2004. 1 Reference ID: 3438270 0 Instructions for Opening Diagram submitted September 27, 2013 (Appendix C) F1111 Prescribing Information submitted September 27, 2013 3 MEDICATION ERROR RISK ASSESSNIENT The Applicant is proposing a combination product that contains Netupitant and Palonosetron. Although Polonosetron is currently marketed, Netupitant is a new molecular entity, and this is the ?rst combination (product containing these two ingredients. The product is supplied in an foil blister pack containing one capsule and packaged in a secondary, (m4) Burgopak. This packaging con?guration is supported by the dosage and administration for this product which is one capsule prior to chemotherapy. We performed a risk assessment of the proposed F1111 Prescribing Information to identify de?ciencies that may lead to medication errors. Additionally, we reviewed the proposed container label and carton labeling to identify areas of improvement. We note that the dosage form is missing and the established name and strength are blended together making each more dif?cult to differentiate. We provide label and labeling recommendations in Section 5 to increase prominence of important information to ensure safe use of the product. 4 CONCLUSIONS DMEPA concludes that the proposed labels and labeling can be improved to increase the readability and prominence of important information on the label and to promote the safe use of the product. 5 RECOMJVIENDATIONS AND COMJVIENTS DMEPA recommends the following be implemented prior to approval of this NDA: 5.1 COMMENTS TO THE APPLICANT 1. Blu'gopak Label and Carton Labeling a. As crurently presented, the dosage form is not present. The established name presentation should include the active ingredient followed by the dosage form. Include the dosage form ?capsules? on all labels and labeling immediately following the active ingredient presentation. Ensure the dosage from presentations is commensurate with the prominence of the active ingredient presentation. b. As currently presented, the established name presentation uses a (ma) font against a white backgrormd which makes it dif?cult to read. Revise the font color to increase the prominence of the established name so that it is commensurate with the prominence of the proprietary name in accordance with 21 CFR 201.10 c. The components of the established name and strength ?netupitant 300 mg, palonoserron 0.5 mg appear blended together making each more dif?cult to differentiate. Revise the presentations of the established name and Reference ID: 3438270 strength so that the established name appears on one line directly beneath the proprietary name and the strength appears on one line directly beneath the established name to increase legibility and differentiation of each, e.g., “Akynzeo” “(netupitant and palonosetron) capsules” “300 mg and 0.5 mg” (b) (4) d. The located to the left of the proprietary name is prominent and may be misinterpreted as part of the proprietary name. Delete this (b) (4) (b) (4) or and relocate away from the proprietary name. 2. Instructions for Opening Diagram The written instructions for opening the BurgoPak on the container label and in the Instructions for Opening Diagram are adequate. However, we recommend revising the pictures accompanying the first two steps, “1. Press buttons A & B together,” and “2. Pull tab with other hand,” to depict the hand holding the Burgopak grasping the Burgopak from the rear (b) (4) rather than where the blister pack emerges. If you have further questions or need clarifications, please contact Mary Chung, Project Manager, at 301-796-0260. 3 Page(s) of Draft Labeling have been Withheld in Full as b4 (CCI/TS) immediately following this page 3 Reference ID: 3438270 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------TERRI WOOD-CUMMINGS 01/17/2014 LUBNA A MERCHANT 01/19/2014 Reference ID: 3438270 RPM FILING REVIEW (Including Memo of Filing Meeting) To be completed for all new NDAs, BLAs, and Efficacy Supplements [except SE8 (labeling change with clinical data) and SE9 (manufacturing change with clinical data] Application Information NDA # 205718 NDA Supplement #: Not applicable (N/A) Efficacy Supplement Type SEN/A Proprietary Name: AKYNZEO Established/Proper Name: netupitant/palonosetron Dosage Form: fixed-dose combination capsule Strengths: 300 mg netupitant/ 0.5 mg palonosetron Applicant: Helsinn Healthcare Agent for Applicant (if applicable): August Consulting Date of Application: 9/27/2013 Date of Receipt: 9/27/2013 Date clock started after UN: N/A PDUFA Goal Date: 9/26/2014 Action Goal Date (if different): N/A Filing Date: 11/26/2013 Date of Filing Meeting: 10/25/2013 Chemical Classification: (1,2,3 etc.) (original NDAs only) 1 Proposed indication(s)/Proposed change(s): Prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of highly emetogenic cancer chemotherapy and moderately emetogenic cancer chemotherapy in adults (acute and delayed CINV HEC and MEC). Type of Original NDA: AND (if applicable) Type of NDA Supplement: X 505(b)(1) 505(b)(2) 505(b)(1) 505(b)(2) If 505(b)(2): Draft the “505(b)(2) Assessment” review found at: http://inside.fda.gov:9003/CDER/OfficeofNewDrugs/ImmediateOffice/UCM027499 and refer to Appendix A for further information. Review Classification: X Standard Priority If the application includes a complete response to pediatric WR, review classification is Priority. If a tropical disease priority review voucher was submitted, review classification is Priority. Resubmission after withdrawal? Part 3 Combination Product? If yes, contact the Office of Combination Products (OCP) and copy them on all Inter-Center consults Version: 08/26/2013 Reference ID: 3413901 Tropical Disease Priority Review Voucher submitted Resubmission after refuse to file? Convenience kit/Co-package Pre-filled drug delivery device/system (syringe, patch, etc.) Pre-filled biologic delivery device/system (syringe, patch, etc.) Device coated/impregnated/combined with drug Device coated/impregnated/combined with biologic Separate products requiring cross-labeling Drug/Biologic Possible combination based on cross-labeling of separate products Other (drug/device/biological product) 1 Fast Track Designation Breakthrough Therapy Designation Rolling Review Orphan Designation Rx-to-OTC switch, Full Rx-to-OTC switch, Partial Direct-to-OTC PMC response PMR response: FDAAA [505(o)] PREA deferred pediatric studies [21 CFR 314.55(b)/21 CFR 601.27(b)] Accelerated approval confirmatory studies (21 CFR 314.510/21 CFR 601.41) Animal rule postmarketing studies to verify clinical benefit and safety (21 CFR 314.610/21 CFR 601.42) Other: PDUFA V Collaborative Review Division (if OTC product): List referenced IND Number(s): IND 73493 Goal Dates/Product Names/Classification Properties YES PDUFA and Action Goal dates correct in tracking system? X NO NA Comment NO NA Comment NA Comment If no, ask the document room staff to correct them immediately. These are the dates used for calculating inspection dates. Are the proprietary, established/proper, and applicant names correct in tracking system? X If no, ask the document room staff to make the corrections. Also, ask the document room staff to add the established/proper name to the supporting IND(s) if not already entered into tracking system. Is the review priority (S or P) and all appropriate classifications/properties entered into tracking system (e.g., chemical classification, combination product classification, 505(b)(2), orphan drug)? For NDAs/NDA supplements, check X the New Application and New Supplement Notification Checklists for a list of all classifications/properties at: http://inside.fda.gov:9003/CDER/OfficeofBusinessProcessSupport/ucm163969.ht m If no, ask the document room staff to make the appropriate entries. Application Integrity Policy YES X Is the application affected by the Application Integrity Policy (AIP)? Check the AIP list at: http://www.fda.gov/ICECI/EnforcementActions/ApplicationIntegrityPolicy/default .htm If yes, explain in comment column. If affected by AIP, has OC/OMPQ been notified of the submission? If yes, date notified: User Fees YES Is Form 3397 (User Fee Cover Sheet) included with authorized signature? X Version: 08/26/2013 Reference ID: 3413901 NO 2 User Fee Status Payment for this application: If a user fee is required and it has not been paid (and it is not exempted or waived), the application is unacceptable for filing following a 5-day grace period. Review stops. Send Unacceptable for Filing (UN) letter and contact user fee staff. X Paid Exempt (orphan, government) Waived (e.g., small business, public health) Not required Payment of other user fees: If the firm is in arrears for other fees (regardless of whether a user fee has been paid for this application), the application is unacceptable for filing (5-day grace period does not apply). Review stops. Send UN letter and contact the user fee staff. X Not in arrears In arrears 505(b)(2) YES NO (NDAs/NDA Efficacy Supplements only) Is the application for a duplicate of a listed drug and eligible for approval under section 505(j) as an ANDA? Is the application for a duplicate of a listed drug whose only difference is that the extent to which the active ingredient(s) is absorbed or otherwise made available to the site of action is less than that of the reference listed drug (RLD)? [see 21 CFR 314.54(b)(1)]. Is the application for a duplicate of a listed drug whose only difference is that the rate at which the proposed product’s active ingredient(s) is absorbed or made available to the site of action is unintentionally less than that of the listed drug [see 21 CFR 314.54(b)(2)]? NA Comment X X X If you answered yes to any of the above questions, the application may be refused for filing under 21 CFR 314.101(d)(9). Contact the 505(b)(2) review staff in the Immediate Office of New Drugs X Is there unexpired exclusivity on any drug product containing the active moiety (e.g., 5-year, 3-year, orphan, or pediatric exclusivity)? Check the Electronic Orange Book at: http://www.accessdata.fda.gov/scripts/cder/ob/default.cfm If yes, please list below: Application No. Drug Name Exclusivity Code Exclusivity Expiration If there is unexpired, 5-year exclusivity remaining on the active moiety for the proposed drug product, a 505(b)(2) application cannot be submitted until the period of exclusivity expires (unless the applicant provides paragraph IV patent certification; then an application can be submitted four years after the date of approval.) Pediatric exclusivity will extend both of the timeframes in this provision by 6 months. 21 CFR 314.108(b)(2). Unexpired, 3year exclusivity may block the approval but not the submission of a 505(b)(2) application. Exclusivity Does another product (same active moiety) have orphan exclusivity for the same indication? Check the Orphan Drug Version: 08/26/2013 Reference ID: 3413901 YES NO NA Comment X 3 Designations and Approvals list at: http://www.accessdata.fda.gov/scripts/opdlisting/oopd/index.cfm X If another product has orphan exclusivity, is the product considered to be the same product according to the orphan drug definition of sameness [see 21 CFR 316.3(b)(13)]? If yes, consult the Director, Division of Regulatory Policy II, Office of Regulatory Policy Has the applicant requested 5-year or 3-year Waxman-Hatch exclusivity? (NDAs/NDA efficacy supplements only) X If yes, # years requested: 5 Note: An applicant can receive exclusivity without requesting it; therefore, requesting exclusivity is not required. X Is the proposed product a single enantiomer of a racemic drug previously approved for a different therapeutic use (NDAs only)? If yes, did the applicant: (a) elect to have the single enantiomer (contained as an active ingredient) not be considered the same active ingredient as that contained in an already approved racemic drug, and/or (b): request exclusivity pursuant to section 505(u) of the Act (per FDAAA Section 1113)? X If yes, contact Mary Ann Holovac, Director of Drug Information, OGD/DLPS/LRB. Format and Content Do not check mixed submission if the only electronic component is the content of labeling (COL). All paper (except for COL) X All electronic Mixed (paper/electronic) CTD Non-CTD Mixed (CTD/non-CTD) If mixed (paper/electronic) submission, which parts of the application are submitted in electronic format? Overall Format/Content YES If electronic submission, does it follow the eCTD guidance? 1 If not, explain (e.g., waiver granted). Index: Does the submission contain an accurate comprehensive index? Is the submission complete as required under 21 CFR 314.50 (NDAs/NDA efficacy supplements) or under 21 CFR 601.2 (BLAs/BLA efficacy supplements) including: X NO NA Comment X X 1 http://www.fda.gov/downloads/Drugs/GuidanceComplianceRegulatoryInformation/Guidances/ucm072349. pdf Version: 08/26/2013 Reference ID: 3413901 4 X legible X English (or translated into English) X pagination X navigable hyperlinks (electronic submissions only) If no, explain. BLAs only: Companion application received if a shared or divided manufacturing arrangement? X If yes, BLA # Forms and Certifications Electronic forms and certifications with electronic signatures (scanned, digital, or electronic – similar to DARRTS, e.g., /s/) are acceptable. Otherwise, paper forms and certifications with hand-written signatures must be included. Forms include: user fee cover sheet (3397), application form (356h), patent information (3542a), financial disclosure (3454/3455), and clinical trials (3674); Certifications include: debarment certification, patent certification(s), field copy certification, and pediatric certification. Application Form YES Is form FDA 356h included with authorized signature per 21 CFR 314.50(a)? X NO NA Comment NO NA Comment NO NA Comment If foreign applicant, a U.S. agent must sign the form [see 21 CFR 314.50(a)(5)]. Are all establishments and their registration numbers listed on the form/attached to the form? X Patent Information YES (NDAs/NDA efficacy supplements only) Is patent information submitted on form FDA 3542a per 21 CFR 314.53(c)? X Financial Disclosure YES Are financial disclosure forms FDA 3454 and/or 3455 included with authorized signature per 21 CFR 54.4(a)(1) and (3)? X Forms must be signed by the APPLICANT, not an Agent [see 21 CFR 54.2(g)]. Note: Financial disclosure is required for bioequivalence studies that are the basis for approval. Version: 08/26/2013 Reference ID: 3413901 The sponsor proposed to utilize NETU-07-07, a phase 2 study to demonstrate the efficacy of the netupitant component of the drug product. The agreement with FDA to utilize this trial as one of the four pivotal clinical trials to support this NDA was made after the completion of the 5 phase 2 study. As such, the collection of Financial Disclosure Forms was obtained retroactively because as a phase 2 study, Financial Disclosure Forms were not required upon initiation of the study. Completed and signed financial disclosure forms were obtained for 181 investigators out of a total of 196 investigators. The sponsor has shown due diligence in obtaining this information to fulfill their financial disclosure requirement for NETU-07-07. Clinical Trials Database YES Is form FDA 3674 included with authorized signature? X NO NA Comment NO NA Comment NO NA Comment If yes, ensure that the application is also coded with the supporting document category, “Form 3674.” If no, ensure that language requesting submission of the form is included in the acknowledgement letter sent to the applicant Debarment Certification YES Is a correctly worded Debarment Certification included with authorized signature? X Certification is not required for supplements if submitted in the original application; If foreign applicant, both the applicant and the U.S. Agent must sign the certification [per Guidance for Industry: Submitting Debarment Certifications]. Note: Debarment Certification should use wording in FD&C Act Section 306(k)(1) i.e.,“[Name of applicant] hereby certifies that it did not and will not use in any capacity the services of any person debarred under section 306 of the Federal Food, Drug, and Cosmetic Act in connection with this application.” Applicant may not use wording such as, “To the best of my knowledge…” Field Copy Certification (NDAs/NDA efficacy supplements only) For paper submissions only: Is a Field Copy Certification (that it is a true copy of the CMC technical section) included? Version: 08/26/2013 Reference ID: 3413901 YES X 6 Field Copy Certification is not needed if there is no CMC technical section or if this is an electronic submission (the Field Office has access to the EDR) If maroon field copy jackets from foreign applicants are received, return them to CDR for delivery to the appropriate field office. Controlled Substance/Product with Abuse Potential YES For NMEs: Is an Abuse Liability Assessment, including a proposal for scheduling, submitted per 21 CFR 314.50(d)(5)(vii)? X NO NA Comment NO NA Comment If yes, date consult sent to the Controlled Substance Staff: 10/8/13 For non-NMEs: Date of consult sent to Controlled Substance Staff : N/A Pediatrics YES PREA X Does the application trigger PREA? If yes, notify PeRC RPM (PeRC meeting is required) 2 Note: NDAs/BLAs/efficacy supplements for new active ingredients, new indications, new dosage forms, new dosing regimens, or new routes of administration trigger PREA. All waiver & deferral requests, pediatric plans, and pediatric assessment studies must be reviewed by PeRC prior to approval of the application/supplement. If the application triggers PREA, are the required pediatric assessment studies or a full waiver of pediatric studies included? X X If studies or full waiver not included, is a request for full waiver of pediatric studies OR a request for partial waiver and/or deferral with a pediatric plan included? If no, request in 74-day letter If a request for full waiver/partial waiver/deferral is included, does the application contain the certification(s) required by FDCA Section 505B(a)(3) and (4)? X If no, request in 74-day letter BPCA (NDAs/NDA efficacy supplements only): X Is this submission a complete response to a pediatric Written Request? If yes, notify Pediatric Exclusivity Board RPM (pediatric exclusivity determination is required) 3 2 3 http://inside.fda.gov:9003/CDER/OfficeofNewDrugs/PediatricandMaternalHealthStaff/ucm027829.htm http://inside.fda.gov:9003/CDER/OfficeofNewDrugs/PediatricandMaternalHealthStaff/ucm027837.htm Version: 08/26/2013 Reference ID: 3413901 7 Proprietary Name YES Is a proposed proprietary name submitted? X NO NA Comment NO NA Comment If yes, ensure that the application is also coded with the supporting document category, “Proprietary Name/Request for Review.” REMS YES X Is a REMS submitted? If yes, send consult to OSE/DRISK and notify OC/ OSI/DSC/PMSB via the CDER OSI RMP mailbox Prescription Labeling Check all types of labeling submitted. Not applicable X Package Insert (PI) X Patient Package Insert (PPI) Instructions for Use (IFU) Medication Guide (MedGuide) X Carton labels X Immediate container labels Diluent Other (specify) YES Is Electronic Content of Labeling (COL) submitted in SPL format? NO NA Comment X If no, request applicant to submit SPL before the filing date. Is the PI submitted in PLR format? 4 X If PI not submitted in PLR format, was a waiver or deferral requested before the application was received or in the submission? If requested before application was submitted, what is the status of the request? If no waiver or deferral, request applicant to submit labeling in PLR format before the filing date. All labeling (PI, PPI, MedGuide, IFU, carton and immediate container labels) consulted to OPDP? MedGuide, PPI, IFU (plus PI) consulted to OSE/DRISK? (send WORD version if available) X Carton and immediate container labels, PI, PPI sent to OSE/DMEPA and appropriate CMC review office (OBP or ONDQA)? X OTC Labeling X Not Applicable Outer carton label Immediate container label Blister card Check all types of labeling submitted. X 4 http://inside fda.gov:9003/CDER/OfficeofNewDrugs/StudyEndpointsandLabelingDevelopmentTeam/ucm0 25576.htm Version: 08/26/2013 Reference ID: 3413901 8 Blister backing label Consumer Information Leaflet (CIL) Physician sample Consumer sample Other (specify) YES NO NA Comment Other Consults YES NO NA Comment Are additional consults needed? (e.g., IFU to CDRH; QT study report to QT Interdisciplinary Review Team) X NO NA Comment Is electronic content of labeling (COL) submitted? If no, request in 74-day letter. Are annotated specifications submitted for all stock keeping units (SKUs)? If no, request in 74-day letter. If representative labeling is submitted, are all represented SKUs defined? If no, request in 74-day letter. All labeling/packaging, and current approved Rx PI (if switch) sent to OSE/DMEPA? If yes, specify consult(s) and date(s) sent: QT Interdisciplinary Review Team: 11/15/2014 SEALD: 11/18/2014 Meeting Minutes/SPAs YES End-of Phase 2 meeting(s)? Date(s): July 20, 2009 X If yes, distribute minutes before filing meeting Pre-NDA/Pre-BLA/Pre-Supplement meeting(s)? Date(s): April 16, 2013 X If yes, distribute minutes before filing meeting Any Special Protocol Assessments (SPAs)? Date(s): January 22, 2010 and July 15, 2010 X If yes, distribute letter and/or relevant minutes before filing meeting Version: 08/26/2013 Reference ID: 3413901 9 ATTACHMENT MEMO OF FILING MEETING DATE: 10/25/2013 BLA/NDA/Supp #: NDA 205718 PROPRIETARY NAME: AKYNZEO ESTABLISHED/PROPER NAME: netupitant/palonosetron DOSAGE FORM/STRENGTH: fixed-dose combination capsule APPLICANT: Helsinn Healthcare PROPOSED INDICATION(S)/PROPOSED CHANGE(S): 1. Prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of highly emetogenic cancer chemotherapy (CINV HEC) 2. Prevention of acute and delayed nausea and vomiting associated with initial and repeat courses of moderately emetogenic cancer chemotherapy (CINV MEC) BACKGROUND: On September 15, 2006, Helsinn Healthcare submitted IND 73493 netupitant palonosetron fixed-dose combination capsule for treatment of chemotherapy induced nausea and vomiting. Helsinn’s clinical development program was discussed at the end-of-phase 2 meeting held on July 20, 2009. A series of Special protocol Assessment (SPA) requests were submitted by the sponsor and Type A SPA meetings were held January 22, 2010 and July 15, 2010. Per discussion from these meetings, four clinical studies (NETU-07-07, PALO-10-01, NETU-08-18, and NETU-10-29) were conducted to support the efficacy and safety of the fixed-dose combination capsule for the prevention of acute and delayed phases of CINV-HEC and CINVMEC. On April 16, 2013, a pre-NDA meeting was held to discuss the results of the phase 3 trials, the content and format of the planned eCTD NDA submission, proposed labeling and the schedule to submit the pediatric study plan. REVIEW TEAM: Discipline/Organization Regulatory Project Management Names RPM: Mary Chung Present at filing meeting? (Y or N) Y CPMS/TL: Brian Strongin Y Cross-Discipline Team Leader (CDTL) Ruyi He Y Clinical Reviewer: Version: 08/26/2013 Reference ID: 3413901 Nancy Snow Y 10 TL: Ruyi He Reviewer: N/A TL: N/A Reviewer: Insook Kim N TL: Sue Chih Lee Y Reviewer: Lisa Kammerman N TL: Freda Cooner Y Reviewer: Ke Zhang Y TL: David Joseph Y Reviewer: N/A TL: N/A Immunogenicity (assay/assay validation) (for BLAs/BLA efficacy supplements) Reviewer: N/A TL: N/A Product Quality (CMC) Reviewer: Raymond Frankewich Y TL: Marie Kowblansky Y Reviewer: N/A TL: N/A Reviewer: Raymond Frankewich Y TL: Marie Kowblansky Y Reviewer: N/A TL: N/A Reviewer: Lisa Khosla Y TL: Lubna Merchant N Reviewer: Yasmin Choudhry N TL: Kendra Worthy N Clinical Microbiology (for antimicrobial products) Clinical Pharmacology Biostatistics Nonclinical (Pharmacology/Toxicology) Statistics (carcinogenicity) Quality Microbiology (for sterile products) CMC Labeling Review Facility Review/Inspection OSE/DMEPA (proprietary name) OSE/DRISK (REMS) Version: 08/26/2013 Reference ID: 3413901 Y 11 OC/OSI/DSC/PMSB (REMS) Bioresearch Monitoring (OSI) Controlled Substance Staff (CSS) Other reviewers Reviewer: N/A TL: N/A Reviewer: Susan Leibenhaut Y TL: Susan Leibenhaut Y Reviewer: Katherine Bonson Y TL: Silvia Calderon N • • Other attendees • • • • • • • Biopharmaceutics: Assadollah Noory, Banu Zonik, Tapash Ghosh (TL) Pharmacometrics: Jingyu (Jerry) Yu OSE/DPV: Christian Cao OMP/PLT: Barbara Fuller PMHS: Erica Radden ODE III: Julie Beitz (Director), Maria Walsh (ADRA), Giuseppe Randazzo (Regulatory Scientist) DGIEP: Donna Griebel (Director), Andrew Mulberg (Deputy director) OSE RPM: Phong (Pete) Do ONDQA RPM: Rebecca McKnight FILING MEETING DISCUSSION: GENERAL • 505(b)(2) filing issues: X Not Applicable o Is the application for a duplicate of a listed drug and eligible for approval under section 505(j) as an ANDA? YES NO o Did the applicant provide a scientific “bridge” demonstrating the relationship between the proposed product and the referenced product(s)/published literature? YES NO Describe the scientific bridge (e.g., BA/BE studies): • Per reviewers, are all parts in English or English translation? Version: 08/26/2013 Reference ID: 3413901 X YES NO 12 If no, explain: • Electronic Submission comments X Not Applicable List comments: CLINICAL Comments: • Clinical study site(s) inspections(s) needed? Not Applicable X FILE REFUSE TO FILE Review issues for 74-day letter X YES NO If no, explain: • Advisory Committee Meeting needed? Comments: YES Date if known: X NO To be determined If no, for an NME NDA or original BLA , include the reason. For example: o this drug/biologic is not the first in its class o the clinical study design was acceptable o the application did not raise significant safety or efficacy issues o the application did not raise significant public health questions on the role of the drug/biologic in the diagnosis, cure, mitigation, treatment or prevention of a disease Reason: Netupitant is an NME but not the first in its class. The application did not raise significant public health questions on the role of the drug in the diagnosis, cure, mitigation, treatment or prevention of a disease. The clinical study design was acceptable and the application did not raise significant safety or efficacy issues. • Not Applicable X FILE REFUSE TO FILE Abuse Liability/Potential Comments: • If the application is affected by the AIP, has the division made a recommendation regarding whether or not an exception to the AIP should be granted to permit review based on medical necessity or public health significance? Review issues for 74-day letter X Not Applicable YES NO Comments: CLINICAL MICROBIOLOGY Version: 08/26/2013 Reference ID: 3413901 X Not Applicable FILE REFUSE TO FILE 13 Comments: Review issues for 74-day letter CLINICAL PHARMACOLOGY Not Applicable X FILE REFUSE TO FILE Comments: • Clinical pharmacology study site(s) inspections(s) needed? Review issues for 74-day letter YES X NO BIOSTATISTICS Not Applicable X FILE REFUSE TO FILE Comments: NONCLINICAL (PHARMACOLOGY/TOXICOLOGY) Review issues for 74-day letter Not Applicable X FILE REFUSE TO FILE Review issues for 74-day letter Comments: IMMUNOGENICITY (BLAs/BLA efficacy supplements only) X Not Applicable FILE REFUSE TO FILE Review issues for 74-day letter Comments: PRODUCT QUALITY (CMC) Comments: Not Applicable X FILE REFUSE TO FILE Review issues for 74-day letter Environmental Assessment • Categorical exclusion for environmental assessment (EA) requested? X YES NO If no, was a complete EA submitted? X YES NO If EA submitted, consulted to EA officer (OPS)? X YES NO Comments: Version: 08/26/2013 Reference ID: 3413901 14 Quality Microbiology (for sterile products) • Was the Microbiology Team consulted for validation of sterilization? (NDAs/NDA supplements only) X Not Applicable YES NO Comments: Facility Inspection Not Applicable • Establishment(s) ready for inspection? X YES NO  Establishment Evaluation Request (EER/TBP-EER) submitted to OMPQ? X YES NO Comments: Facility/Microbiology Review (BLAs only) Comments: X Not Applicable FILE REFUSE TO FILE Review issues for 74-day letter CMC Labeling Review Comments: Review issues for 74-day letter APPLICATIONS IN THE PROGRAM (PDUFA V) (NME NDAs/Original BLAs) • Were there agreements made at the application’s pre-submission meeting (and documented in the minutes) regarding certain late submission components that could be submitted within 30 days after receipt of the original application? • If so, were the late submission components all submitted within 30 days? • What late submission components, if any, arrived after 30 days? Version: 08/26/2013 Reference ID: 3413901 N/A YES X NO YES NO N/A 15 • Was the application otherwise complete upon submission, including those applications where there were no agreements regarding late submission components? X YES NO • Is a comprehensive and readily located list of all clinical sites included or referenced in the application? X YES NO • Is a comprehensive and readily located list of all manufacturing facilities included or referenced in the application? X YES NO REGULATORY PROJECT MANAGEMENT Signatory Authority: Julie Beitz, Director, ODE III Date of Mid-Cycle Meeting (for NME NDAs/BLAs in “the Program” PDUFA V): February 12, 2014 REGULATORY CONCLUSIONS/DEFICIENCIES The application is unsuitable for filing. Explain why: X The application, on its face, appears to be suitable for filing. Review Issues: X No review issues have been identified for the 74-day letter. Review issues have been identified for the 74-day letter. Review Classification: X Standard Review Priority Review ACTIONS ITEMS X Ensure that any updates to the review priority (S or P) and classifications/properties are entered into tracking system (e.g., chemical classification, combination product classification, 505(b)(2), orphan drug). If RTF, notify everybody who already received a consult request, OSE PM, and Product Quality PM (to cancel EER/TBP-EER). If filed, and the application is under AIP, prepare a letter either granting (for signature by Center Director) or denying (for signature by ODE Director) an exception for review. Version: 08/26/2013 Reference ID: 3413901 16 BLA/BLA supplements: If filed, send 60-day filing letter If priority review: • notify sponsor in writing by day 60 (For BLAs/BLA supplements: include in 60-day filing letter; For NDAs/NDA supplements: see CST for choices) X • notify OMPQ (so facility inspections can be scheduled earlier) Send review issues/no review issues by day 74 X Conduct a PLR format labeling review and include labeling issues in the 74-day letter X Update the PDUFA V DARRTS page (for NME NDAs in the Program) BLA/BLA supplements: Send the Product Information Sheet to the product reviewer and the Facility Information Sheet to the facility reviewer for completion. Ensure that the completed forms are forwarded to the CDER RMS-BLA Superuser for data entry into RMS-BLA one month prior to taking an action [These sheets may be found in the CST eRoom at: http://eroom.fda.gov/eRoom/CDER2/CDERStandardLettersCommittee/0 1685f ] Other Version: 08/26/2013 Reference ID: 3413901 17 Appendix A (NDA and NDA Supplements only) NOTE: The term "original application" or "original NDA" as used in this appendix denotes the NDA submitted. It does not refer to the reference drug product or "reference listed drug." An original application is likely to be a 505(b)(2) application if: (1) it relies on published literature to meet any of the approval requirements, and the applicant does not have a written right of reference to the underlying data. If published literature is cited in the NDA but is not necessary for approval, the inclusion of such literature will not, in itself, make the application a 505(b)(2) application, (2) it relies for approval on the Agency's previous findings of safety and efficacy for a listed drug product and the applicant does not own or have right to reference the data supporting that approval, or (3) it relies on what is "generally known" or "scientifically accepted" about a class of products to support the safety or effectiveness of the particular drug for which the applicant is seeking approval. (Note, however, that this does not mean any reference to general information or knowledge (e.g., about disease etiology, support for particular endpoints, methods of analysis) causes the application to be a 505(b)(2) application.) Types of products for which 505(b)(2) applications are likely to be submitted include: fixed-dose combination drug products (e.g., heart drug and diuretic (hydrochlorothiazide) combinations); OTC monograph deviations (see 21 CFR 330.11); new dosage forms; new indications; and, new salts. An efficacy supplement can be either a (b)(1) or a (b)(2) regardless of whether the original NDA was a (b)(1) or a (b)(2). An efficacy supplement is a 505(b)(1) supplement if the supplement contains all of the information needed to support the approval of the change proposed in the supplement. For example, if the supplemental application is for a new indication, the supplement is a 505(b)(1) if: (1) The applicant has conducted its own studies to support the new indication (or otherwise owns or has right of reference to the data/studies), (2) No additional information beyond what is included in the supplement or was embodied in the finding of safety and effectiveness for the original application or previously approved supplements is needed to support the change. For example, this would likely be the case with respect to safety considerations if the dose(s) was/were the same as (or lower than) the original application, and. (3) All other “criteria” are met (e.g., the applicant owns or has right of reference to the data relied upon for approval of the supplement, the application does not rely Version: 08/26/2013 Reference ID: 3413901 18 for approval on published literature based on data to which the applicant does not have a right of reference). An efficacy supplement is a 505(b)(2) supplement if: (1) Approval of the change proposed in the supplemental application would require data beyond that needed to support our previous finding of safety and efficacy in the approval of the original application (or earlier supplement), and the applicant has not conducted all of its own studies for approval of the change, or obtained a right to reference studies it does not own. For example, if the change were for a new indication AND a higher dose, we would likely require clinical efficacy data and preclinical safety data to approve the higher dose. If the applicant provided the effectiveness data, but had to rely on a different listed drug, or a new aspect of a previously cited listed drug, to support the safety of the new dose, the supplement would be a 505(b)(2), (2) The applicant relies for approval of the supplement on published literature that is based on data that the applicant does not own or have a right to reference. If published literature is cited in the supplement but is not necessary for approval, the inclusion of such literature will not, in itself, make the supplement a 505(b)(2) supplement, or (3) The applicant is relying upon any data they do not own or to which they do not have right of reference. If you have questions about whether an application is a 505(b)(1) or 505(b)(2) application, consult with your OND ADRA or OND IO. Version: 08/26/2013 Reference ID: 3413901 19 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature. --------------------------------------------------------------------------------------------------------/s/ ---------------------------------------------------MARY H CHUNG 11/26/2013 Reference ID: 3413901