CENTER FOR DRUG EVALUATION AND
RESEARCH

APPLICATION NUMBER:

205641Orig1s000
CLINICAL PHARMACOLOGY AND
BIOPHARMACEUTICS REVIEW(S)

 OFFICE OF CLINICAL PHARMACOLOGY:
CLINICAL PHARMACOLOGY REVIEW
NDA

205641

Submission Date:

June 26, 2013

Brand Name:

Asmanex® HFA

Generic Name:

Mometasone furoate

Clinical Pharmacology
Reviewer:

Dinko Rekić, M.Sc., Ph.D.

Clinical Pharmacology Team
Leader:

Satjit Brar, Pharm.D., Ph.D.

Pharmacometrics Reviewer:

Dinko Rekić, M.Sc., Ph.D.

Pharmacometrics Team
Leader:

Liang Zhao, Ph.D.

OCP Division:

DCP2

OND Division:

DPARP (OND-570)

Sponsor:

Merck

Application type

505 (b)(1) non-NME

Dosing regimen:

Two inhalations twice daily (morning and evening)

Dosage form

Metered Dose Inhaler (MDI)

Strengths:

100 or 200 µg BID

Indication:

Maintenance treatment of asthma as prophylactic
therapy in patients 12 years of age and older

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 1 of 22

 Table of Contents
1

EXECUTIVE SUMMARY ........................................................................................ 3
1.1 Recommendations ................................................................................................ 3
1.2 Phase IV commitments......................................................................................... 3
2 SUMMARY OF CLINICAL PHARMACOLOGY AND BIOPHARMACEUTICS
FINDINGS .......................................................................................................................... 4
2.1 Regulatory background ........................................................................................ 4
2.1.1
Clinical pharmacology bridging ................................................................... 4
2.1.2
Comparison of efficacy with Asmanex Twistinhaler ................................... 5
3
QUESTION BASED REVIEW .................................................................................. 6
3.1 General Attributes/Background............................................................................ 6
3.2 What is the pertinent regulatory background of ASMANEX HFA? ................... 6
3.3 What are the proposed mechanism of action and therapeutic indications?.......... 6
3.4 What are the proposed dosages and routes of administration? ............................ 6
3.5 List the in vitro and in vivo Clinical Pharmacology and Biopharmaceutics
studies and the clinical studies with PK and/or PD information submitted in the NDA
or BLA ............................................................................................................................ 7
3.6 General Clinical Pharmacology ........................................................................... 7
3.7 What are the design features of the clinical pharmacology and biopharmaceutics
studies and the clinical studies used to support dosing or claims? ................................. 7
3.8 What is the basis for selecting the product dose?................................................. 7
3.8.1
Study C97-208 .............................................................................................. 8
3.8.2
Study C97-225 .............................................................................................. 8
3.8.3
Study I97-200................................................................................................ 9
3.8.4
Study C97-224 .............................................................................................. 9
3.8.5
Reviewer’s analysis of dose-response relationship..................................... 10
3.9 Is the dose and dosing regimen selected consistent with the known E-R
relationship? .................................................................................................................. 16
3.10 What is previously known about the pharmacokinetics of MF .......................... 16
3.11 What is the impact of chronic MF dosing on cortisol suppression .................... 17
3.12 General Biopharmaceutics ................................................................................. 17
3.12.1 What is the relative bioavailability of the proposed product and Dulera ... 17
4
PRELIMINARY LABELING RECOMMENDATIONS......................................... 19
4.1 Clinical Pharmacology ....................................................................................... 19
5 APPENDIX ............................................................................................................... 20
5.1 Annotated Proposed Package insert from the sponsor ....................................... 20

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 2 of 22

 1 EXECUTIVE SUMMARY
The sponsor is seeking approval for a new formulation (metered dose inhaler [MDI]) of
the inhaled corticosteroid mometasone furoate (MF) with the proposed trade name
Asmanex HFA®. MF formulated in a dry powder inhaler (DPI) is an approved product
with the trade name Asmanex Twistinhaler®.
Studies supporting efficacy of Asmanex HFA have been conducted as part of the
Dulera® program where MF MDI was used as active control. Dulera (NDA 22518) is an
approved combination product of MF and formoterol fumarate (F), formulated in a MDI.
Clinical pharmacology studies supporting the application where conducted using Dulera
(MF/F MDI), Asmanex Twistinhaler (MF DPI) or Asmanex HFA (MF MDI).
This review has determined that there is no evidence of formulation or metabolic
interaction between MF and F when formulated in a MDI. Hence, the clinical
pharmacology studies conducted with co-formulated MF and F in a MDI are relevant to
this application. The sponsor has fulfilled the clinical pharmacology requirements of a
NDA and no further clinical pharmacology studies are warranted.
Reviewer’s independent analysis of the FEV 1 endpoint, using phase II trials from the
Dulera program, shows that the two treatments (Asmanex HFA and Asmanex
Twistinhaler) have equivalent response when administered at the same dose.
1.1 Recommendations
The Office of Clinical Pharmacology/Division of Clinical Pharmacology-2 (OCP/DCP-2)
has reviewed NDA 205641and finds it acceptable, provided that a mutually satisfactory
agreement can be reached between the sponsor and the agency regarding the language in
the package insert.
1.2 Phase IV commitments
None

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 3 of 22

 2

SUMMARY OF CLINICAL PHARMACOLOGY AND
BIOPHARMACEUTICS FINDINGS
The focus of this review is to determine if the clinical pharmacology studies conducted
during the Dulera program (MF, MF/F MDI) and the Asmanex Twistinhaler program
(MF DPI) are relevant to this application.
Additionally, dose finding phase II trials from the Dulera program and the Asmanex
Twistinhaler program are re-analyzed to compare the treatment effect of Asmanex
Twistinhaler (MF DPI) and Asmanex HFA (MF MDI).
2.1 Regulatory background
The proposed product is an inhaled corticosteroid (mometasone furoate [MF]) indicated
for maintenance treatment of asthma as prophylactic therapy in patients 12 years of age
and older. The proposed doses are 200 µg and 400 µg BID delivered by two actuations.
Each actuation delivers one dose of 100 µg or 200 µg, depending on the presentation.
Mometasone furoate is currently approved for treatment of asthma in two formulations:
1) a dry powder inhalation (DPI) device with the trade name Asmanex Twistinhaler® and
2) as part of a combination product with the long-acting β2-agonist formoterol fumarate
(F) with the trade name Dulera®. MF, delivered by a metered dose inhaler (MDI), was
used as an active control in development of Dulera. The sponsor is seeking approval for
MF MDI formulation, with the proposed trade name Asmanex HFA, based on the studies
conducted during the Dulera program as well as the Asmanex Twistinhaler program.
Clinical pharmacology findings
2.1.1 Clinical pharmacology bridging
There are no statistically or clinically relevant differences in mometasone plasma
exposure, following Asmanex HFA (MF MDI) or Dulera (MF/F MDI) administration.
No pharmacokinetic or formulation interactions between formoterol and mometasone
have been found, therefore, results from clinical pharmacology studies of mometasone
when co-formulated with formoterol are relevant and applicable to this application.
Mometasone plasma exposure is significantly lower when administered by a MDI
(Asmanex HFA) device compared to a DPI (Asmanex Twistinhaler) device. Based on
difference in systemic exposure, Asmanex Twistinhaler represents worst case scenario of
Asmanex HFA in regards to concentration dependent systemic safety profile. Below is a
list of items that are supported by findings from the Dulera program and the Asmanex
Twistinhaler program.
Items supported by Dulera program (MF/F, MDI):


HPA axis (Study PO3705)

Items supported by Dulera program (MF, MDI):




Dose and dose regimen (phase II and Phase III trials)
Oral prednisone reduction in subjects with severe asthma (Study C97-224)
Efficacy and safety in geriatrics and pediatrics (Phase III trials)

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 4 of 22

 Items supported by Asmanex Twistinhaler program (MF, DPI):





Drug-Drug interaction with the CYP3A4 inhibitor ketoconazole (Study I98-216)
Growth inhibition in pediatrics (Study C98-384)
Hepatic Impairment (Study C98-291)
Reduction in bone mineral density (Study C98-302)

Some studies supporting this application where conducted more than 15 years ago.
Consequently, the systemic exposure of mometasone was not measurable with
technology available at that time. The hepatic impairment study was only able to measure
increased number of observations above lower limit of detection (LOQ) with increasing
level of hepatic impairment. The ketoconazole interaction study applied a similar
approach. However, in addition to increased exposure to mometasone, a higher degree of
cortisol suppression was detected. Because systemic mometasone exposure following
Asmanex HFA is significantly lower than following Asmanex Twistinhaler
administration, it is possible that reduction in bone mineral density as well as growth
inhibition in pediatrics will be less severe with the new product. Sponsor’s choice to
reference studies conducted with Asmanex Twistinhaler is appropriate as they can
represent a worst case scenario.
2.1.2 Comparison of efficacy with Asmanex Twistinhaler
A reviewer initiated analysis of phase II Asmanex HFA trials (trials (I97-200, C97-225,
C97-224, C97-208) and Asmanex Twistinhaler phase II trial (C96-134) has determined
that the mean treatment effect for the two regimens is not expected to be different when
administered at the same dose.

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 5 of 22

 3
3.1

QUESTION BASED REVIEW
General Attributes/Background

3.2 What is the pertinent regulatory background of ASMANEX HFA?
The active ingredient of the product has previously been approved as a single ingredient
product in Asmanex Twistinhaler (DPI) as well as part of a combination product with
formoterol (Dulera) MDI. Relevant products to this review are listed in Table 1.
Asmanex HFA is essentially the same product as Dulera but without the formoterol
component..
Table 1. Table of products related to this submission.
Product

Active ingredients Patient
Population

D evice

D ate

A smanex
Tw istinhaler

mometasone
furoate

A sthma in
patients of 12
years and older

DPI

A pproved
03/ 30/ 2005

A smanex
Tw istinhaler

mometasone
furoate

A sthma in
patients of 4 years
and older

DPI

A pproved
02/ 01/ 2008

Dulera

mometasone
furoate and
formoterol

A sthma in
patients of 12
years and older

M DI

A pproved
06/ 22/ 2010

Dulera

mometasone
furoate and
formoterol

COPD

M DI

Complete
response
01/ 27/ 2012

3.3 What are the proposed mechanism of action and therapeutic indications?
Mometasone furoate is a corticosteroid with anti-inflammatory effects. The precise
mechanism of action in asthma is unknown. The proposed indication is maintenance
treatment of asthma as prophylactic therapy in patients 12 years of age and older.
3.4 What are the proposed dosages and routes of administration?
Asmanex HFA is an inhaled corticosteroid delivered via a hydrofluoroalkane (HFA)propelled pressurized metered dose inhaler (pMDI). Two dosage strengths are proposed:
100 µg and 200 µg administered as 2 inhalations twice daily (BID). This review refers to
the dose strengths 100 µg and 200 µg. The dose strength correspond to doses of 200 µg
and 400 µg delivered by two actuations. The starting dose is dependent on previous
corticosteroid therapy. The proposed dosages are summarized in Table 2.

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 6 of 22

 Table 2. Recommended dosages for Asmanex HFA
Previous Therapy

Recommended dose

Total delivered dose

Inhaled medium-dose corticosteroids 100 µg 2 inhalations BID

200 µg BID

Inhaled high-dose corticosteroids

200 µg 2 inhalations BID

400 µg BID

Oral corticosteroids

200 µg 2 inhalations BID

400 µg BID

List the in vitro and in vivo Clinical Pharmacology and Biopharmaceutics
studies and the clinical studies with PK and/or PD information submitted in
the NDA or BLA
No new studies have been submitted in this application. For complete list of clinical
pharmacology studies in the Dulera program please see the clinical pharmacology review
of Dulera (NDA 22518) by Drs. Fan and Zhao dated May 21, 2009.
3.5

Sponsor is referencing studies in Dulera and the Asmanex Twistinhaler program. Below
is a list of studies supported by the two programs.
Items supported by Dulera program (MF/F, MDI):


HPA axis (Study PO3705)

Items supported by Dulera program (MF, MDI):




Dose and dose regiment (phase II and Phase III trials)
Oral prednisone reduction in Subjects with severe asthma (Study C97-224)
Efficacy and safety in geriatrics and pediatrics (Phase III trials)

Items supported by Asmanex Twistinhaler program (MF, DPI):




3.6

Drug-Drug interaction with CYP3A4 inhibitor: ketoconazole (Study I98-216)
Growth inhibition in pediatrics (Study C98-384)
Hepatic Impairment (Study C98-291)
Reduction in bone mineral density (Study C98-302)
General Clinical Pharmacology

3.7

What are the design features of the clinical pharmacology and
biopharmaceutics studies and the clinical studies used to support dosing or
claims?
Reference is made to Dr. Limb’s review dated May 21, 2010 as well as sections 3.8.1 to
3.8.4.
3.8 What is the basis for selecting the product dose?
Dose selection for mometasone is based on trials performed in the Dulera program as
well as the doses in the Asmanex Twistinhaler program. The following studies are

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 7 of 22

 invoked by the sponsor in support of the proposed doses: C97208, C97225, I97200 and,
C97224. These studies have been reviewed previously by Dr. Limb in her clinical review
dated May 21, 2010. Table 3 lists number of subjects and doses tested in the trials.
Table 3. List of studies supporting the proposed dose strengths of MF MDI, with the
number of subjects per dose group
Trial ID

50 µg
BID

100 µg
*

BID

200 µg

400 µg

600 µg

800 µg

BID

BID

BID

BID

74

73

*

C97-208**

71

73

C97-225**

58

57

I97-200**

176

182

C97-224
Total number of
subjects

176

312

72
59

176
42

129

Placebo

292

73

43

38

43

169

The doses are delivered by two actuations BID.
* The proposed strengths.
** An additional active control arm was included in this trial.

3.8.1 Study C97-208
Randomized, active and placebo controlled, parallel group, double blind trial in patient
with moderate to severe asthma ages 12 to 81. Number of subjects in each arm is shown
in Table 3. In addition to arms shown in Table 3, beclomethasone dipropionate MDI 168
µg was used as an active control. The main efficacy point was FEV1, which was not a
trough value. Sponsor claims these values to be comparable to trough values because of
majority of measurements were performed within 1 to 4 hours of the AM dose. All active
treatments were superior compared to placebo, supporting the efficacy of MF 50 µg, 200
µg, 400 µg, and 600 µg dose strengths against placebo. FEV1 increased by 6.5% from
baseline for the active control arm at week 12. In order to compare efficacy across trials,
week 12 FEV1 values were used in Figure 1.
3.8.2 Study C97-225
Randomized, active and placebo controlled, parallel group, double blind trial in patient
with moderate to severe asthma ages 12 years and older. In addition to those in Table 3,
beclomethasone dipropionate MDI 168 µg was used as an active control. The primary
efficacy endpoint was FEV1. All active treatments were superior compared to placebo,
supporting the efficacy of MF 50 µg, 200 µg dose strengths against placebo. In order to
compare efficacy across trials, week 12 FEV1 values were used in Figure 1. FEV1
increased by 8.2% from baseline for the active control arm at week 12.

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 8 of 22

 3.8.3 Study I97-200
Randomized, active-control, evaluator blind, parallel group, phase III trial in patients
with moderate to severe asthma. Fluticasone propionate MDI 250 µg was included as
active comparator. The study did not include a placebo arm. The main efficacy point was
FEV1, which was not a trough value. In order to compare efficacy across trials, week 12
FEV1 values were used in Figure 1.
3.8.4 Study C97-224
Randomized, placebo controlled, double-blind, parallel group, phase III trial in patients
with moderate to severe asthma. The main efficacy endpoint was change in daily
prednisolone requirement. FEV1 was evaluated as a secondary endpoint. All active
treatments were superior compared to placebo, supporting the efficacy of MF 400 µg,
800 µg dose strengths against placebo. In order to compare efficacy across trials, week 12
FEV1 values were used in Figure 1.
The studies chosen by the sponsor to support the proposed doses have some important
differences: 1) Not all studies were placebo-controlled (i.e., I97-200); 2) two different
active comparators were used in studies C97-225 and C97-208 (beclomethasone
dipropionate) and in study I97-200 (fluticasone propionate); 3) Studies C97-208, C97225, and I97-200 were conducted in patients with moderately severe asthma while study
C97-224 was conducted in patients with severe asthma; 4) The primary endpoint was
FEV1 in studies C97-208, C97-225, and I97-200 while FEV1 was designated as
secondary endpoint in study I97-200; 5) It is uncertain if all FEV1 values are considered
trough values; 6) study I97-200 is essentially a corticosteroid reduction study while
studies C97-208, C97-225, and I97-200 are dose ranging studies.
FEV1 change from baseline at week 12 is plotted verses dose strength for all studies,
Figure 1.

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 9 of 22

 Figure 1. I ntegrated visualization of dose-response relationship for studies C97-208, C97-224,
C97-225, and I 97-200. D ose zero refers to placebo arm. Effect is defined as improvement in
FEV 1 at week 12. D ose strengths of 100 µg and 200 µg proposed for marketing in this
submission. The doses are delivered by two actuations, BI D .

3.8.5 Reviewer’s analysis of dose-response relationship
Purpose
The purpose of this analysis is to compare the efficacy of Asmanex Twistinhaler and
Asmanex HFA utilizing data from different studies and drug development programs.
Data: Asmanex HFA
Mean percent FEV1 change from baseline at week 12 was extracted from Section 2.7.3 –
Summary of Clinical Efficacy for studies C97-208, C97-224, C97-225, and I97-200. The
respective studies are summaries in section 3.8. The data is based on the per protocol
population.
Data: Asmanex Twistinhaler
Mean percent FEV1 change from baseline at week 12 was extracted from Table 1, page
13 for study C96-134 from Dr. Gebert’s statistical review of NDA 21067 (dated
September 14, 1999). It is assumed that the data is based on the per protocol population.
Methods
Statistical software R (2.15.2) and the package “Dose-Finding” (0.9-9) was used to
estimate the dose-response relationship 1. Model selection for non-hierarchical as well as
hierarchical models was based on Akaike information Criterion (AIC). Evaluated models
and their corresponding AIC values are shown in Table 4.

1

Björn B et al. Journal of Statistical Software (2009).
N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 10 of 22

 Statistical uncertainty in model selection should be accounted for when making
inferences. If ignored, this uncertainty may lead to over-confident predictions and riskier
decisions than initially believed 2. Model averaging is a method where a number of prespecified models are fit to the data and evaluated based on either the Akaike Information
Criteria (AIC) or Bayesian information criterion (BIC). Predictions from each model are
weighted against their respective AICi or BICi according to Equation 1. The final model
average prediction will be based on all models in proportion to the individual model
weight (wi). Individual model weights are shown in Table 4.
𝑤𝑖 =

exp(−0.5 𝐴𝐼𝐶𝑖 )

∑𝑖 (exp(−0.5𝐴𝐼𝐶𝑖 ))

Equation 1

The mean estimate and confidence intervals for the model average predictions were
obtained by repeating the following steps for all models:
1. Fit all models to the data;
2. Sample 10,000 model parameters based on the estimated variance-covariance
matrix;
3. Simulate 10,000 trials with the sampled model parameters;
4. Sample x number of trials where x is the product of wi and number of simulated
trials.
The 50th, the 10th, and the 90th percentile were obtained based on the weighted combined
simulations.
This meta-analysis was based on reported mean change in FEV1 at week 12. Data from
multiple studies (C97-208, C97-224, C97-225, and I97-200) was pooled. Although, dosearm sample size ranged from 38 to 182 subjects, all study arms were given equal
weighting. No attempt was made to estimate inter study variability. Homoscedastic
variance and normally distributed data are assumed. Based on the purpose of this
analysis, these assumptions are found acceptable.
Results
Based on AIC, the Linear in log model was chosen as the final model. Parameter
estimates of the final model with their associated estimates of uncertainty are shown in
Table 5. Figure 2 and Figure 3 illustrate the estimated dose-effect relationship based on
the final model, and the model averaging approach. Parameter estimates and their
respective relative standard error, based on the variance -covariance matrix, were used to
generate the confidence interval for the predicted response.
Table 6 summarizes the estimated treatment effect with the final model and the model
averaging approach. Effect is measured as percent change in FEV1 from baseline at week
12. The distributions of the predicted effect stratified by dose (based on the model
averaging approach) are shown in Figure 4. The probability to show an improvement
over baseline (2.31 L) of 140 mL or more is 93.59 and 95.95 percent for the 100 µg and

2

Buckland, et al., Biometrics (1997).
N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 11 of 22

 the 200 µg dose strengths, respectively. There is no evidence of dose separation between
the 100 and the 200 µg dose.
In Figure 3, mean treatment effect at week 12 following Asmanex Twistinhaler (study
C96-134) administration is shown as triangles. The data from study C96-134 was not
used for model building purposes; it is plotted in figure 3 for illustrative purposes only.
The derived dose-response relationship for Asmanex HFA appears to be representative of
the Asmanex Twistinhaler dose-response observations, suggesting that the mean
treatment effect for the two regimens is not expected to be different when administered at
the same dose.
Conclusions
Asmanex Twistinhaler response is not expected to be significantly different from
Asmanex HFA response, if not equivalent.
Similar conclusions can be made regardless of the approach employed (model averaging
or parametric modeling). The higher dose strength shows a numerical superiority
compared to the lower dose. However, confidence intervals of the mean effect are
overlapping and dose separation appears to be minimal if at all present. In fact, the
second best model (based on AIC) suggests a complete flat dose response curve for all
doses.

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 12 of 22

 Table 4. Evaluated dose-response models
Model

Equation

Model
weight

AIC

Linear
Model

-48.14

0.00

Quadratic
Model

-53.62

0.00

Logistic
Model

-58.38

0.05

Sigmoid
Emax
Model

-58.89

0.06

Beta
model

-59.78

0.09

Emax
model

-60.88

0.16

-61.79

0.26

-62.55

0.38

Piesewise
flat dose
response
model

𝑖𝑓 𝑑𝑜𝑠𝑒 = 𝑝𝑙𝑎𝑐𝑒𝑏𝑜: 𝑓(𝑑, 𝜃) = 𝐸𝑝

𝑖𝑓 𝑑𝑜𝑠𝑒 ≠ 𝑝𝑙𝑎𝑐𝑒𝑏𝑜: 𝑓(𝑑, 𝜃) = 𝐸𝑡

Linear in
log
Model*

AIC: Akaike information criterion (lower is better), d: dose variable, E0: placebo effect, Emax: maximum
effect (for Beta model: within tested dose range), ED50: Dose giving half of the maximum effect, h, Hill
parameter, determining the steepness of the model at the ED50, off: fixed value used to avoid problems
with dose=0. Scal: fixed scale parameter, β: parameter of the quadratic model, δ: for exponential model:
Parameter, controlling the convexity of the model, for Linear and lin-log model: Slope parameter, Logistic
model: Parameter controlling determining the steepness of the curve. E1 Slope parameter for exponential
model. * Selected as the final model.

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 13 of 22

 Table 5. Parameter estimates and their associated precision for the final (linear in
log)
Linear in log model
(AIC -62.55)

Parameter
Estimate

Relative Standard error (%)

0.064

9.46

δ (%/log(µg))

0.00398

17.11

Residual standard error

0.0226

NA

E0 (%)

E0 is the estimated placebo effect at week 12 measured as change in FEV1 from baseline in percent, δ is
the slope parameter estimating change in effect with increasing dose.Doses are delivered by two
actuations, BID. Effect is measured as percent change in FEV1 from baseline at week 12

Table 6. Estimates of treatment effect based on parametric models and model
averaging approach.
Mean estimated effect (CI: 90%)
Method
100 µg BID
Model Averaging

Final model
(lin-log [AIC: -62.55])

8.20%
(6.81-9.20)
8.24%
(7.16-9.31)

189.42 mL

190.34 mL

200 µg BID
8.51%
(7.29-9.46)
8.51%
(7.40-9.62)

196.58 mL

196.58 mL

Mean estimated effect is measured as percent change from baseline. Absolute change from baseline is
calculated from the combined mean baseline value of 2.31 L from studies: C97-208, C97-224, C97-225,
and I97-200.

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 14 of 22

 Figure 2. Estimated dose-response relationship based on the final model. D ose refers to dosage
strength in µg. Response is defined as fraction FEV 1 change from baseline. Grey circles
represent the mean change from baseline for a dose group at week 12 of the study. Lines
represent the mean predicted response with confidence interval (CI : 90%).

Figure 3. Estimated dose-response relationship based on the model averaging approach. D ose
refers to dosage strength in µg. Response is defined as fraction FEV 1 change from baseline.
Circles represent the mean change from baseline for a dose group at week 12 for in a study.
Lines and the shaded grey area represent the mean predicted response with confidence
interval (CI : 90%). D ata from Study C96-134 (Asmanex Twistinhaler) are superimposed in the
plot (teal triangles) but where not used in generation of the model.

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 15 of 22

 Figure 4. Weighted distributions of treatment effect for the 100 µg and the 200 µg dose
strength. The red line indicates an improvement over baseline of 6.06 % or 140 mL. The
probability to reach a treatment effect of 140 mL or greater is 93.59 and 95.95 percent forth the
100 µg and the 200 µg dose strengths, respectively.

3.9

Is the dose and dosing regimen selected consistent with the known E-R
relationship?
Systemic exposure of mometasone is of unknown importance to treatment effect. Dose
selection based on efficacy is currently only informed by dose-response analysis.
3.10 What is previously known about the pharmacokinetics of MF
Oral bioavailability of mometasone has been determined to be less than 1%. Systemic
exposure following inhalation is therefore likely to originate from local lung absorption.
Following 28 days of inhaled administration of 400 µg mometasone BID, mean plasma
concentrations at steady state ranged from 94 to 114 pg/mL and mean time to maximum
concentrations ranged from 1 to 2.5 hours.
Intravenous administration of mometasone displays bi-phasic disposition with a mean
terminal half-life of 5 hours. Steady state volume of distribution is estimated to 152 liters.
Plasma protein binding was reported to be ~98% in the concentration range of 5 to 500
ng/mL.
In vitro studies have identified CYP3A4 as the major route of metabolism. However, no
major metabolites have been identified. Radioactive mometasone is mainly excreted in
feces (74%) and do some extend in urine (8%). Unchanged mometasone was not
associated with radioactivity in urine, i.e. it is unlikely that un-metabolized mometasone
is excreted in urine.
For detailed clinical pharmacology summary, the reader is referred to the clinical
pharmacology review of Dulera (NDA 22518) by Drs. Fan and Zhao dated May 21,
2009.

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 16 of 22

 3.11 What is the impact of chronic MF dosing on cortisol suppression
As no new clinical studies have been conducted and the sponsor is referring to the
corticosteroid suppression studies submitted under the Dulera applications; detailed
review of those studies can be found in the clinical pharmacology review of Dulera
(NDA 22518) by Drs. Fan and Zhao dated May 21, 2009.
There is a lack of interaction between MF and F when they are administered together.
Because of this, results of corticosteroid suppression studies conducted with MF/F MDI
(Dulera) device are meaningful to this application. Please see section 3.12.1 for
discussion on relative bioavailability between MF MDI and MF/F MDI.
3.12 General Biopharmaceutics
3.12.1 What is the relative bioavailability of the proposed product and Dulera
There are no statistically or clinically relevant differences in mometasone plasma
exposure, following Asmanex HFA (MF MDI) or Dulera (MF/F MDI) administration.
Because no pharmacokinetic or formulation interaction between formoterol and
mometasone has been found, results from clinical pharmacology studies of mometasone
when formulated with formoterol are relevant and applicable to this application.
The current submission does not include new clinical studies. For general discussion
about the studies’ design, please see clinical pharmacology review of Dulera (NDA
22518) by Drs. Fan and Zhao dated May 21, 2009.
The sponsor is supporting this application by making reference to the following studies in
the Dulera program: P03658 and P05644. In addition to those trials the reviewer has
identified trial PO4275, also from the Dulera program, to be relevant to this application
Table 7.
Clinical pharmacology trials supporting this interaction intend to show the following:
•

Lack of pharmacokinetic interaction between MF and F (PO3658)

•

Lack of formulation interaction on MF when MF and F are formulated (MDI),
(PO3658)

•

MF systemic exposure is not dosage-form proportional (P05644)

Figure 5 summarizes the above-mentioned studies in an integrated forest plot. The
implication of the results in study PO3658 are that pharmacokinetic characteristics of MF
when delivered via MDI as a single ingredient product are similar to MF when coformulated with F in a metered dose inhaler. These results provide the necessary bridge
that allows the sponsor to rely on the studies conducted with MF/F in the Dulera
program.
Study PO3658 suggest that 4 inhalations of 100/5 µg MF/F and 2 inhalations of 200/10
µg MF/F result in different exposure of MF. These results are relevant for single
ingredient MF MDI because trial PO4275 established that there is no pharmacokinetic
interaction between F and MF. These results may indicate that the 100 µg and the 200 µg
dose strength may not be used interchangeably when adjusted by number of inhalations.
One possible explanation to these finding is that the relative absorption surface increases
N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 17 of 22

 following four verses versus two inhalations. The increase relative absorption area would
result in increased bioavailability.
The original Dulera program relied, in part, on safety and efficacy of the approved
Asmanex Twistinhaler program. The clinical pharmacology trials in the Dulera
submission aimed to provide a link between the Asmanex Twistinhaler and Dulera. Trial
PO4275 investigated the relative bioavailability of MF when administered via a single
ingredient DPI device and via a MF/F MDI device. The results of trial PO4275 suggest
that systemic exposure of MF is significantly lower following MDI administration
compared to DPI administration Table 7. These results suggest that the two formulations
MDI and DPI fail to deliver a bioequivalent dose of MF. Because of the findings in trial
PO3658, the results are believed to be a due to formulation and/or device and not due to a
metabolic interaction between F and MF.
Table 7. Formulation and drug interaction trials relevant to this submission.
Trial ID

Treatments arms

Population

Results

PO36581 1) MF 800 µg MDI
2) F 20 µg MDI
3) MF 800 µg MDI+F 20 µg
MDI
4) MF 800 µg/F 20 µg MDI

Healthy
volunteers

There is a lack of interaction
between MF and F when they are
administered concomitantly via a
MDI device.

P042751

Healthy
volunteers

MF AUC(0-12hr) is approximately
52% to 25% lower following
MDI administration compared
with DPI administration.

Healthy
volunteers

MF dosage form proportionality
could not be concluded.
Treatment 1) resulted in 75%
(95%CI: [48-108]) higher
exposure compared of MF
compared to treatment 3).
Treatment 2) and 3) resulted in
56% difference in exposure.

1) MF 800 µg/F 20 µg MDI
2) MF 800 µg DPI

PO56441 1) 8 puffs x (50 μg/5 μg
MF/F) MDI2
2) 4 puffs x (100 μg/5 μg
MF/F) MDI2
3) 2 puffs x (200 μg/5 μg
MF/F) MDI2

MF: mometasone furoate, F: formoterol, AUC: area under the concentration-time curve, MDI: metered
dose inhaler, DPI: dry powder inhaler. 1 Reference is made to clinical pharmacology review by Drs. Fan
and Zhao dated May 21, 2009. 2 Total dose of MF was 800 μg in all treatments.

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 18 of 22

 a)

b)

Figure 5. Integrated summary of results from studies P03658, P05644, and P04275. Figure
5a) shows the mean AUC ratio with 90% confidence intervals, figure 5b) shows the mean
Cmax ration with 90% confidence intervals.

4

PRELIMINARY LABELING RECOMMENDATIONS

4.1 Clinical Pharmacology
The proposed label is acceptable form a clinical pharmacology perspective.

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 19 of 22

 5 APPENDIX

5.1 Proposed Package insert from the sponsor
12 CLINICAL PHARMACOLOGY

12.1Mechanism of Action

Mometasone furoate is a corticosteroid demonstrating potent anti-in?ammatory activity. The
precise mechanism of corticosteroid action on asthma is not known. Inflammation is an
important component in the pathogenesis of asthma. Corticosteroids have been shown to
have a wide range of inhibitory effects on multiple cell types mast cells, eosinophils,
neutrophils, macrophages, and and mediators histamine, eicosanoids,
leukotrienes, and cytokines) involved in inflammation and in the asthmatic response. These
anti-in?ammatory actions of corticosteroids may contribute to their ef?cacy in asthma.

Mometasone furoate has been shown in vitro to exhibit a binding af?nity for the human
glucocorticoid receptor, which is approximately 12 times that of dexamethasone, 7 times that
of triamcinolone acetonide, 5 times that of budesonide, and 1.5 times that of ?uticasone. The
clinical signi?cance of these ?ndings is unknown.

12.2Pharmacodynamies

HPA Axis Effects

The effects of inhaled mometasone furoate administered via ASMANEX HFA on adrenal
function have not been directly evaluated. However, the effects of inhaled mometasone
furoate administered on adrenal function were evaluated in two clinical trials in
patients with asthma. As no evidence of a pharmacokinetic drug interaction between
mometasone furoate and formoterol was observed when the two drugs were administered
the HPA axis effects from mm are applicable to ASMANEX HFA. 
clinical development program, HPA-axis function was assessed by 24-hour plasma
cortisol AUC. Although both these trials have open-label design and contain a small number
of subjects per treatment arm, results from these trials taken together demonstrated
suppression of 24-hour plasma cortisol AUC for (m4) 200 mcg/5 compared to
placebo consistent with the known systemic effects of inhaled corticosteroid.

In a 42-day, open-label, placebo- and active-controlled study, the mean change from baseline

plasma cortisol was 22% and 34% lower compared to placebo for the
100 mcg/5 200 meg/5 (n=15) and ?uticasone

propronate/salmeterol xinafoate 230 mcg/21 (n=16) treatment groups, respectively.

In a 52-week, open-label safety study, the mean plasma cortisol was 
29.6%, 16.7%, and 32.2% lower from baseline for the 100 mcg/5 

(m4) 200 meg/5 ?uticasone propionate/salmeterol xinafoate 125/25 
and ?uticasone propionate/salmeterol xinafoate 250/25 (n=11) treatment groups,
respectively.

The potential effect of mometasone furoate via a dry powder inhaler (DPI) on the HPA axis
was assessed in a 29-day study. A total of 64 adult patients with mild to moderate asthma
were randomized to one of 4 treatment groups: mometasone furoate DPI 440 twice
daily, mometasone furoate DPI 880 twice daily, oral prednisone 10 mg once daily, or
placebo. The 30-minute stimulation serum cortisol concentration on Day 29
was 23.2 mcg/dL for the mometasone furoate DPI 440 twice daily group and 20.8
mcg/dL for the mometasone furoate DPI 880 twice daily group, compared to 14.5
mcg/dL for the oral prednisone 10 mg group and 25 mcg/dL for the placebo group. The
difference between mometasone furoate DPI 880 twice daily (twice the maximum
recommended dose) and placebo was statistically signi?cant.

DA205641 Page 20 of 22

ClinPhann.Review_Asmanex_l .2.docx

Reference ID: 3471550

12.3 Pharmacokinetics
As no evidence of a pharmacokinetic drug interaction between mometasone furoate and
(b) (4)
formoterol was observed when the two drugs were administered from
the
(b) (4)
pharmacokinetics information from
is applicable to ASMANEX HFA.
Absorption
Healthy Subjects: Following oral inhalation of single doses of ASMANEX HFA, mometasone
furoate was absorbed in healthy subjects with median Tmax values ranging from 0.50 to
2 hours. Following single-dose administration of higher than recommended dose of
ASMANEX HFA (4 inhalations of ASMANEX HFA 200 mcg) in healthy subjects, the
arithmetic mean (CV%) Cmax and AUC(0-tf) values for mometasone furoate were 53 (102)
pg/mL and 992 (80) pg•hr/mL, respectively. Studies using oral dosing of labeled and
unlabeled drug have demonstrated that the oral systemic bioavailability of mometasone
furoate is negligible (<1%).
(b) (4)
Asthma Patients: Following oral inhalation of single and multiple doses of the
mometasone furoate was absorbed in asthma patients with median Tmax values ranging from
(b) (4)
1 to 2 hours. Following single-dose administration of
400 mcg/10 mcg, the
arithmetic mean (CV%) Cmax and AUC(0-12 hr) values for mometasone furoate were 20 (88)
pg/mL and 170 (94) pg•hr/mL, respectively, while the corresponding estimates following twice
(b) (4)
daily dosing of
400 mcg/10 mcg at steady-state were 60 (36) pg/mL and 577 (40)
pg•hr/mL.

Distribution
Based on the study employing a 1000 mcg inhaled dose of tritiated mometasone furoate
inhalation powder in humans, no appreciable accumulation of mometasone furoate in the red
blood cells was found. Following an intravenous 400 mcg dose of mometasone furoate, the
plasma concentrations showed a biphasic decline, with a mean steady-state volume of
distribution of 152 liters. The in vitro protein binding for mometasone furoate was reported to
be 98% to 99% (in a concentration range of 5 to 500 ng/mL).
Metabolism
Studies have shown that mometasone furoate is primarily and extensively metabolized in the
liver of all species investigated and undergoes extensive metabolism to multiple metabolites.
In vitro studies have confirmed the primary role of human liver CYP3A4 in the metabolism of
this compound; however, no major metabolites were identified. Human liver CYP3A4
metabolizes mometasone furoate to 6-beta hydroxy mometasone furoate.
Excretion
Following an intravenous dosing, the terminal half-life was reported to be about 5 hours.
Following the inhaled dose of tritiated 1000 mcg mometasone furoate, the radioactivity is
excreted mainly in the feces (a mean of 74%), and to a small extent in the urine (a mean of
8%) up to 7 days. No radioactivity was associated with unchanged mometasone furoate in
the urine. Absorbed mometasone furoate is cleared from plasma at a rate of approximately
12.5 mL/min/kg, independent of dose. The effective t½ for mometasone furoate following
inhalation with DULERA was 25 hours in healthy subjects and in patients with asthma.
Special Populations
Hepatic/Renal Impairment: There are no data regarding the specific use of ASMANEX HFA in
patients with hepatic or renal impairment.
A study evaluating the administration of a single inhaled dose of 400 mcg mometasone
furoate by a dry powder inhaler to subjects with mild (n=4), moderate (n=4), and severe (n=4)
hepatic impairment resulted in only 1 or 2 subjects in each group having detectable peak
plasma concentrations of mometasone furoate (ranging from 50-105 pg/mL). The observed
N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 21 of 22

 peak plasma concentrations appear to increase with severity of hepatic impairment; however,
the numbers of detectable levels were few.
Gender and Race: Specific studies to examine the effects of gender and race on the
pharmacokinetics of ASMANEX HFA have not been specifically studied.
Geriatrics: The pharmacokinetics of ASMANEX HFA have not been specifically studied in the
elderly population.
Drug-Drug Interactions
A single-dose crossover study was conducted to compare the pharmacokinetics of 4
(b) (4)
inhalations of the following: mometasone furoate MDI, formoterol MDI,
(mometasone furoate/formoterol fumarate MDI), and mometasone furoate MDI plus
formoterol fumarate MDI administered concurrently. The results of the study indicated that
there was no evidence of a pharmacokinetic interaction between mometasone furoate and
formoterol.
Inhibitors of Cytochrome P450 Enzymes: Ketoconazole: In a drug interaction study, an
inhaled dose of mometasone furoate 400 mcg delivered by a dry powder inhaler was given to
24 healthy subjects twice daily for 9 days and ketoconazole 200 mg (as well as placebo)
were given twice daily concomitantly on Days 4 to 9. Mometasone furoate plasma
concentrations were <150 pg/mL on Day 3 prior to coadministration of ketoconazole or
placebo. Following concomitant administration of ketoconazole, 4 out of 12 subjects in the
ketoconazole treatment group (n=12) had peak plasma concentrations of mometasone
furoate >200 pg/mL on Day 9 (211-324 pg/mL). Mometasone furoate plasma levels appeared
to increase and plasma cortisol levels appeared to decrease upon concomitant administration
of ketoconazole.

N DA 205641
ClinPharm.Review_Asmanex_1.2.docx

Reference ID: 3471550

Page 22 of 22

 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed
electronically and this page is the manifestation of the electronic
signature.
--------------------------------------------------------------------------------------------------------/s/
---------------------------------------------------DINKO REKIC
03/14/2014
LIANG ZHAO
03/14/2014
SATJIT S BRAR
03/14/2014

Reference ID: 3471550

 CLINICAL PHARMACOLOGY AND BIOPHARMACEUTICS
FILING FORM/CHECKLIST FOR NDA/BLA or Supplement

Office of Clinical Pharmacology
New Drug Application Filing and Review Form
New formulation of mometasone furoate.
Information
NDA/BLA Number
OCP Division (I, II, III, IV, V)
Medical Division
OCP Reviewer

OCP Team Leader
Pharmacometrics Reviewer
Date of Submission
Estimated Due Date of OCP Review
Medical Division Due Date
PDUFA Due Date

205641

Brand Name
Generic Name
Drug Class

II
Division of Pulmonary, Allergy,
and Rheumatology Products
Dinko Rekic, Ph.D.

Indication(s)

Satjit Brar, Pharm.D., Ph.D.
NA
June 26, 2013

Dosage Form
Dosing Regimen
Route of Administration
Sponsor
Priority Classification

Information
Asmanex HFA
mometasone furoate
Corticosteroid
Maintenance treatment
of asthma as
prophylactic therapy in
patients 12 years of age
and older
Metered dose inhaler
200 or 400 μg BID
Oral Inhalation
Merck
standard

4/27/14

Clin. Pharm. and Biopharm. Information
“X” if included
at filing

Number of
studies
submitted

Number of
studies
reviewed

Critical Comments If any

STUDY TYPE
Table of Contents present and sufficient to
locate reports, tables, data, etc.
Tabular Listing of All Human Studies
HPK Summary
Labeling
Reference Bioanalytical and Analytical
Methods
I. Clinical Pharmacology
Mass balance:
Isozyme characterization:
Blood/plasma ratio:
Plasma protein binding:
Pharmacokinetics (e.g., Phase I) -

x
x
x
x

x

Healthy Volunteerssingle dose:
multiple dose:

X
x

2
1

P03658/P05644
P04275

single dose:
multiple dose:

X
X

2
3

P05643/P06144
P03705/P04689

x

1

P05644

X
X

3
2

P03658/P04275/P05642
P03658/ P04275

Patients-

Dose proportionality fasting / non-fasting single dose:
fasting / non-fasting multiple dose:
Drug-drug interaction studies In-vivo effects on primary drug:
In-vivo effects of primary drug:
In-vitro:

File name: 5_Clinical Pharmacology and Biopharmaceutics Filing Form/Checklist for NDA
205641
Reference ID: 3360327

 CLINICAL PHARMACOLOGY AND BIOPHARMACEUTICS
FILING FORM/CHECKLIST FOR NDA/BLA or Supplement
Subpopulation studies ethnicity:
gender:
pediatrics:
geriatrics:
renal impairment:
hepatic impairment:
PD Phase 2:
Phase 3:

x
x

1
4

P06144 (only F)
P04073/P04334/P04431/P04705

PK/PD Phase 1 and/or 2, proof of concept:
Phase 3 clinical trial:
Population Analyses Data rich:
Data sparse:
II. Biopharmaceutics
Absolute bioavailability
Relative bioavailability solution as reference:
alternate formulation as reference:
Bioequivalence studies traditional design; single / multi dose:
replicate design; single / multi dose:
Food-drug interaction studies
Bio-waiver request based on BCS
BCS class
Dissolution study to evaluate alcohol induced
dose-dumping
III. Other CPB Studies
Genotype/phenotype studies
Chronopharmacokinetics
Pediatric development plan
Literature References
Total Number of Studies

14

On initial review of the NDA/BLA application for filing:

Content Parameter
Criteria for Refusal to File (RTF)
1 Has the applicant submitted bioequivalence data comparing tobe-marketed product(s) and those used in the pivotal clinical
trials?
2 Has the applicant provided metabolism and drug-drug
interaction information?
3 Has the sponsor submitted bioavailability data satisfying the
CFR requirements?
4 Did the sponsor submit data to allow the evaluation of the
validity of the analytical assay?
5 Has a rationale for dose selection been submitted?
6 Is the clinical pharmacology and biopharmaceutics section of
the NDA organized, indexed and paginated in a manner to
allow substantive review to begin?
7 Is the clinical pharmacology and biopharmaceutics section of

Yes No N/A

Comment

x

x
x
x
x
x

x

File name: 5_Clinical Pharmacology and Biopharmaceutics Filing Form/Checklist for NDA
205641
Reference ID: 3360327

 CLINICAL PHARMACOLOGY AND BIOPHARMACEUTICS
FILING FORM/CHECKLIST FOR NDA/BLA or Supplement
8

the NDA legible so that a substantive review can begin?
Is the electronic submission searchable, does it have
appropriate hyperlinks and do the hyperlinks work?

x

Criteria for Assessing Quality of an NDA (Preliminary Assessment of Quality)
Data
9 Are the data sets, as requested during pre-submission
x
discussions, submitted in the appropriate format (e.g.,
CDISC)?
10 If applicable, are the pharmacogenomic data sets submitted in
x
the appropriate format?
11 Is the appropriate pharmacokinetic information submitted?
12 Has the applicant made an appropriate attempt to determine
reasonable dose individualization strategies for this product
(i.e., appropriately designed and analyzed dose-ranging or
pivotal studies)?
13 Are the appropriate exposure-response (for desired and
undesired effects) analyses conducted and submitted as
described in the Exposure-Response guidance?
14 Is there an adequate attempt by the applicant to use exposureresponse relationships in order to assess the need for dose
adjustments for intrinsic/extrinsic factors that might affect the
pharmacokinetic or pharmacodynamics?
15 Are the pediatric exclusivity studies adequately designed to
demonstrate effectiveness, if the drug is indeed effective?
16 Did the applicant submit all the pediatric exclusivity data, as
described in the WR?
17 Is there adequate information on the pharmacokinetics and
exposure-response in the clinical pharmacology section of the
label?

x
x

18 Are the clinical pharmacology and biopharmaceutics studies of
appropriate design and breadth of investigation to meet basic
requirements for approvability of this product?
19 Was the translation (of study reports or other study
information) from another language needed and provided in
this submission?

x

x

Orally inhaled
product with low
systemic exposure

x

x
x
x

x

File name: 5_Clinical Pharmacology and Biopharmaceutics Filing Form/Checklist for NDA
205641
Reference ID: 3360327

 CLINICAL PHARMACOLOGY AND BIOPHARMACEUTICS
FILING FORM/CHECKLIST FOR NDA/BLA or Supplement
IS THE CLINICAL PHARMACOLOGY SECTION OF THE APPLICATION FILEABLE?
_YES__
If the NDA/BLA is not fileable from the clinical pharmacology perspective, state the reasons and provide
comments to be sent to the Applicant.
Please identify and list any potential review issues to be forwarded to the Applicant for the 74-day letter.

Reviewing Clinical Pharmacologist

Date

Team Leader/Supervisor

Date

File name: 5_Clinical Pharmacology and Biopharmaceutics Filing Form/Checklist for NDA
205641
Reference ID: 3360327

 --------------------------------------------------------------------------------------------------------This is a representation of an electronic record that was signed
electronically and this page is the manifestation of the electronic
signature.
--------------------------------------------------------------------------------------------------------/s/
---------------------------------------------------DINKO REKIC
08/20/2013
SATJIT S BRAR
08/20/2013

Reference ID: 3360327