Pulmonary Allergy Drugs Advisory Committee Meeting

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Pulmonary Allergy Drugs Advisory Committee Meeting

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Title: Pulmonary Allergy Drugs Advisory Committee Meeting

1
Pulmonary - Allergy Drugs Advisory Committee
Meeting

January 17, 2002
FLOVENT DISKUS NDA 20-833
ADVAIR DISKUS NDA 21-077

2
FLOVENT DISKUS and ADVAIR DISKUS

David Wheadon, MD
Senior Vice President, Regulatory Affairs
GlaxoSmithKline

3
sNDAs forFLOVENT DISKUS and ADVAIR DISKUS

INDICATION
Long term, twice-daily maintenance treatment of
Chronic Obstructive Pulmonary Disease (including
emphysema and chronic bronchitis)

4
SEREVENT(salmeterol xinafoate)

Serevent Inhalation Aerosol approved for COPD,
1998
Approval sought for Serevent Diskus for the
maintenance treatment of bronchospasm associated
with COPD

5
FLOVENT(fluticasone propionate)

Currently Approved in US for maintenance
treatment of asthma
Approved for COPD in 67 countries outside US
Worldwide exposure estimate - 14.4 million
patient years
Approval sought for Flovent Diskus for
maintenance treatment of COPD at doses of 250mcg
and 500mcg BID

6
ADVAIR DISKUS(fluticasone propionate
andsalmeterol inhalation powder)

Currently approved for maintenance treatment of
asthma
Worldwide exposure estimate - 1.4 million patient
years
Approval sought for maintenance treatment of COPD
at doses of 250/50mcg and 500/50mcg BID

7
Impact of COPD in the US

Affects an estimated 21.7 million Americans1
6.5 Million Diagnosed
4.3 Million Treated With Prescription Medications
The fourth leading cause of death2
114,000 deaths in 19982
Third leading cause of death by 20203
Annual cost gt30 billion2
14.7 billion in direct healthcare costs
15.7 billion in indirect healthcare costs

1Data on file (analysis of NHANES III data),
GlaxoSmithKline. 2National Center for Health
Statistics, National Health Interview Survey,
1998. Information cited in American Lung
Association, trends in Chronic bronchitis and
Emphysema Morbidity and Mortality, December,
2000. 3Murray CJL and Lopez AD, eds. The Global
Burden of Disease. Vol. 1. 1996362.
8
Global Initiative for ChronicObstructiveLungDis
ease
Global Initiative for Chronic Obstructive Lung
Disease. Global Strategy for the Diagnosis,
Management, and Prevention of Chronic Obstructive
Pulmonary Disease NHLBI/WHO Workshop Report.
Bethesda, Md National Heart, Lung, and Blood
Institute, National Institutes of Health March
2001. NIH publication 2701A.
9
Clinical Effects of ICS in COPD

Reference N Duration Treatment/Day Outcome
Nishimura et al., 1999 30 4 w BDP 3000mcg ? FEV1,
? Sx
OBrien et al., 2001 24 6 w BDP 1500mcg FEV1
preserved
Thompson et al., 1992 30 6 w BDP 1000mcg ? FEV1,
? bronchitis
Weiner et al., 1995 30 6 w BUD 800mcg ? FEV1, ?
prn med
Weiner et al., 1999 168 6 w BUD 1600mcg ? FEV1, ?
prn med
Auffarth et al., 1991 21 8 w BUD 1600mcg ?
dyspnea
Kerstjens et al., 1993 39 12 w BDP 800mcg ? FEV1
Dompeling et al., 1992 28 52 w BDP 800mcg ? PEF,
? Sx
Paggiaro et al., 1998 281 24 w FP 1000mcg ?
FEV1, ? exac
ISOLDE, 2000 751 3 Y FP 1000mcg ? FEV1, ? QoL, ?
exac
Euroscope, 1999 1277 3 Y BUD 800mcg ? FEV1, ?
exac
Lung Health II, 2000 1116 3 Y TAA 1200mcg ? Sx ,
? exac
Sin Tu, 2001 22620 Varied ? morbidity,
mortality

10
Current Use of ICS for COPDPrescription Data
from July 2001

40 of all COPD patients were prescribed ICS
therapy
46 of all patients prescribed 2 or more COPD
maintenance medications (any medication other
than albuterol)
72 prescribed an ICS
57 prescribed an ICS a maintenance
bronchodilator
17 prescribed Advair

Source NDC Health, July 2001
11
SUMMARY

COPD is a serious public health issue
Considerable unmet medical needs
New treatment options are needed

12
Order of GSK Presentation

Scientific and Clinical Rationale
Dr. Malcolm Johnson (15 minutes)
Clinicians Perspective
Dr. James Donohue (15 minutes)
Clinical Efficacy and Safety
Dr. Tushar Shah (45 minutes)
Conclusion and Q A
Dr. David Wheadon

13
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14
Scientific and Clinical Rationale

Malcolm Johnson, PhD
Global Director of Respiratory Science
GlaxoSmithKline

15
Pathology of COPD
Inflammation
Structural Changes
AirwayObstruction
16
Pathophysiological Features of COPD
Airway Obstruction
StructuralChanges
Inflammation
Smooth muscle contraction Increased cholinergic
tone Loss of elastic recoil
Increased Neutrophils,macrophages, CD8
lymphocytes. Elevated IL-8, TNFa? Protease/anti-pr
oteaseimbalance
Alveolar destruction Collagen deposition Glandular
hypertrophy Airway fibrosis
Symptoms ? FEV1 Exacerbations
17
Inhaled Corticosteroids

Do inhaled corticosteroids reduce inflammation in
COPD?
Are inhaled corticosteroids effective treatment
for COPD?

18
Anti-Inflammatory Effects of ICS in COPD

Reference N Duration Treatment/Day Outcome
Balbi 8 6 w BDP 1500mcg ? BAL neutrophils, IL-8
et al., 2000 and MPO
Confalonieri 24 8 w BDP 1500mcg ? Sputum
neutrophils et al., 1998
Llewellyn-Jones 17 8 w FP 1500mcg ? Sputum
neutrophil et al., 1996 chemotactic
activity
Thompson 30 6 w BDP 1000mcg Improvement in
bronchial et al., 1992 cell counts and
epithelial lining fluid proteins
Yildiz 18 8 w FP 1500mcg ? Sputum neutrophilset
al., 2000
Hattotuwa 37 12 w FP 1000mcg ? Biopsy CD8/CD4
et al., 1999, 2000 Tcell ratio and mast cells
Verhoeven 20 24 w FP 1000mcg ? Biopsy CD8 Tcells
and et al., 1999 eosinophils
Keatings 13 2 w BUD 1600mcg No change in total
and et al.,1996 differential cell counts or
TNF?, ECP, EPO and MPO
Culpitt 13 4 w FP 1000mcg No change in sputum et
al., 1999 neutrophils, IL-8 or SLPI
OBrien 5 6 w BDP 400mcg No change in sputum et
al., 2001 neutrophils

19
Fluticasone Propionate Reduces Total Cell Counts
and Neutrophils in the Sputum of COPD Patients
Total Cell Counts
Neutrophils

x106 cells/g

percent
Placebo
FP 1500 mcg/day

Plt0.05
Yildiz et al. Respiration. 2000 6771-76.
20
ICS (FP) Reduces Inflammation in COPD
Airway Obstruction
StructuralChanges
Inflammation
ICS (FP) Positive Effect
?
Smooth muscle contraction Increased cholinergic
tone Loss of elastic recoil
Increased Neutrophils,macrophages, CD8
lymphocytes. Elevated IL-8, TNFa? Protease/anti-pr
oteaseimbalance
Alveolar destruction Collagen deposition Glandular
hypertrophy Airway fibrosis
Symptoms ? FEV1 Exacerbations
21
Inhaled Corticosteroids

Do inhaled corticosteroids reduce inflammation in
COPD?
Are inhaled corticosteroids effective treatment
for COPD?

22
Clinical Effects of ICS in COPD

Reference N Duration Treatment/Day Outcome
Nishimura et al., 1999 30 4 w BDP 3000mcg ? FEV1,
? Sx
OBrien et al., 2001 24 6 w BDP 1500mcg FEV1
preserved
Thompson et al., 1992 30 6 w BDP 1000mcg ? FEV1,
? bronchitis
Weiner et al., 1995 30 6 w BUD 800mcg ? FEV1, ?
prn med
Weiner et al., 1999 168 6 w BUD 1600mcg ? FEV1, ?
prn med
Auffarth et al., 1991 21 8 w BUD 1600mcg ?
dyspnea
Kerstjens et al., 1993 39 12 w BDP 800mcg ? FEV1
Dompeling et al., 1992 28 52 w BDP 800mcg ? PEF,
? Sx
Paggiaro et al., 1998 281 24 w FP 1000mcg ?
FEV1, ? exac
ISOLDE, 2000 751 3 Y FP 1000mcg ? FEV1, ? QoL, ?
exac
Euroscope, 1999 1277 3 Y BUD 800mcg ? FEV1, ?
exac
Lung Health II, 2000 1116 3 Y TAA 1200mcg ? Sx ,
? exac
Sin Tu, 2001 22620 Varied ? morbidity,
mortality
Keatings et al., 1999 13 2 w BUD 1600mcg No
? PFT, Sx, prn med
Culpitt et al., 1999 13 4 w FP 1000mcg No ?
PFT, Sx
Engel et al., 1989 18 12 w BUD 800mcg No ?
PFT, SxWatson et al., 1992 14 12 w BUD
1200mcg No ? PFT, Sx
Bourbeau et al., 1998 79 28 w BUD 1600mcg No
? PFT, Sx, QoL

23
Reduced Risk of Mortality and Repeat
Hospitalization with Inhaled Corticosteroids
Adapted from Sin DD, Tu JV. Am J Respir Crit
Care Med 2001164580-584
24
Fluticasone Propionate Significantly Improves
Pre-dose FEV1 in COPD
Plt0.01
Plt0.02
? FEV1 (L)
Week
Paggiaro et al. Lancet. 1998 351773-780.
25
Collection of Exacerbation Data in Paggiaro et
al., 1998

Exacerbation history at least 1/ year (treated
by physician or hospital) for previous 3 years
Exacerbation worsening of COPD symptoms
requiring changes to normal treatment
Exacerbation severity
Mild patient self-managed at home
Moderate patient treated by a physician
Severe patient hospitalized
Multiple exacerbations requiring OCS were allowed

Paggiaro et al. Lancet. 1998 351773-780.
26
Fluticasone Propionate Reduces Moderate/Severe
Exacerbations in COPD
Treatment Group
Fluticasone Placebo propionate (n139) (n142)
Number of exacerbations Total 111 76 Number of
Patients with one or moreexacerbations Total
51 45 Mild 7 (14) 17 (38) Moderate/severe 44
(86) 27 (60)
Each patient may have experienced more than one
exacerbation. plt0.001.
Paggiaro et al. Lancet. 1998 351773-780.
27
Inhaled Steroids in Obstructive Lung Disease in
Europe (ISOLDE)
FP MDI 500mcg BID
Corticosteroid Withdrawal
PlaceboRun-in
Placebo BID
2 Months
3 yrs
N 751 Reversibility lt10 predicted Mean FEV1
50 at baseline
Burge PS et al. Br Med J. 20003201297-1303.
28
FP Improves Post-bronchodilator FEV1 Response in
COPD ISOLDE Study
Adapted from Burge PS et al. Br Med J.
20003201297-1303.
29
FP Reduces Median Annual Exacerbation Rate
ISOLDE Study
1.32
p0.026
O.99
Exacerbations/patient/year
Burge PS et al., Br Med J. 20003201297-1303
30
FP Slows the Decline in Quality of Life as
Measured by SGRQ ISOLDE Study
An increase in score reflects a decrease in
quality of life. St Georges Respiratory
Questionnaire Burge PS et al. Br Med J.
20003201297-1303.
31
ICS (FP) Reduces Inflammation in COPD
Airway Obstruction
StructuralChanges
Inflammation
ICS (FP) Positive Effect
?
Smooth muscle contraction Increased cholinergic
tone Loss of elastic recoil
Increased Neutrophils,macrophages, CD8
lymphocytes. Elevated IL-8, TNFa? Protease/anti-pr
oteaseimbalance
Alveolar destruction Collagen deposition Glandular
hypertrophy Airway fibrosis
? Symptoms ? FEV1 ? Exacerbations
32
Salmeterol in COPD
33
Salmeterol is a Long-Acting Bronchodilator in COPD
P lt .001 salmeterol vs placebo. Adapted from
Mahler DA et al. Chest. 1999115957-965.
34
Salmeterol Reduces Airway Obstruction in COPD
Airway Obstruction
StructuralChanges
Inflammation
Salmeterol Positive Effect
Smooth muscle contraction Increased cholinergic
tone Loss of elastic recoil
Increased Neutrophils,macrophages, CD8
lymphocytes. Elevated IL-8, TNFa? Protease/anti-pr
oteaseimbalance
Alveolar destruction Collagen deposition Glandular
hypertrophy Airway fibrosis

Symptoms
? FEV1
Exacerbations

35
Combined Effects of Salmeterol and FP in COPD
Salmeterol FP
?
Airway Obstruction
StructuralChanges
Inflammation
Increased Neutrophils,macrophages, CD8
lymphocytes. Elevated IL-8, TNFa? Protease/anti-pr
oteaseimbalance
Smooth muscle contraction Increased cholinergic
tone Loss of elastic recoil
Alveolar destruction Collagen deposition Glandular
hypertrophy Airway fibrosis

? Symptoms
? FEV1
? Exacerbations

36
Corticosteroids Increase RespiratoryMucosal
Beta2-receptors

0.45
0.40
0.35
0.30
beta2-receptor/actin ratio
0.25
0.20
0.15
0.10
plt0.04

0.05
0
Baseline
BDP 100mcg for 3 days
Baraniuk et al AJRCCM 155 704-710(1997)
37
Salmeterol Potentiates the Effect of FP on
TNF?-induced IL8 Release fromAirway Smooth
Muscle Cells
IL8 (pg/ml)
P lt0.01
?
(0.1 µM)
(1 µM)
(0.1 µM)
Adapted from Pang L, and Knox AJ. Am J Respir
Cell Mol Biol. 2000 23 79-85.
38
Rationale for CombiningFP with Salmeterol

Fluticasone propionate is an effective inhaled
anti-inflammatory corticosteroid with clinical
benefit in COPD.
Salmeterol is a long-acting b2-adrenoceptor
agonist with demonstrated efficacy in COPD.
Each molecule influences a different aspect of
COPD pathophysiology, so together they provide a
broad therapeutic cover.
There is some evidence of interaction between
these molecules which may be important in
improving the overall efficacy of the combination.

39
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40
Clinicians Perspective

James F. Donohue, MD
Chief, Pulmonary and Critical Care
MedicineUniversity of North Carolina, Chapel Hill

41
Overview

Diagnosis of COPD
Evaluating treatment effects in COPD
FEV1
Other measures
GOLD guidelines
Clinicians Perspective

42
Diagnosis of COPD

Clinically based on
Smoking history
Age
Symptoms
Persistent airflow obstruction (spirometry)
FEV1 post bronchodilator lt 80 predicted
FEV1 / FVC lt 70
The presence of reversibility does not exclude a
diagnosis of COPD

43
Bronchodilator Response in COPDIntermittent
Positive Pressure Breathing Trial (IPPB)

Evaluated the BD response to inhaled
isoproteronol in 985 subjects with COPD (asthma
excluded)
Pre and post- bronchodilator FEV1 evaluated every
3 months for 3 yrs.
Key demographics
Age 60.9
Male 79
Smoking Status
54 pack yrs
40 current smokers
FEV1 ( predicted) 36

Anthonisen, et al. Am Rev Respir Dis,
198613314-20.
44
Bronchodilator Response in COPD IPPB Trial

Approximately half of the subjects were
reversible at screening (gt12 increase in FEV1
over baseline)
In subjects non-reversible at screening (lt10
increase in FEV1)
30 of these subjects had a gt15 increase in FEV1
at each subsequent test day
68 of these subjects had a gt15 increase in FEV1
on at least one of the 7 follow-up test days

Annals of Internal Medicine, 198399612-620.
Anthonisen, et al. Am Rev Respir Dis,
1986133814-819.
45
Demographic and Reversibility Data from Clinical
Trials in COPD

Salmeterol Combivent Formoterol
(n816) (n1067) (n780)
Age 63 64 63
male 68 69 75
Pack yr 63 na 42
FEV1 L ( pred) 1.25 (40) 0.99 (36) 1.3 (45)
Pts Rev 62 68-73 42

Data on file SLGA 4004, SLGA 4005, Chest 1994
1051411-1419. Chest 1999 115966-971. Am J
Respir Crit Care Med. Vol 165. p. 778-784, 2001.
46
Efficacy Measures Used to Assess Treatment
Response in COPD

Spirometry (FEV1)
Objective, reproducible
Diagnostic and prognostic
Other Measures
Health Status (QOL)
Symptoms
Exacerbations

47
FEV1 Response withCombivent on Day 85
Ipratropium Albuterol (n 173)Albuterol (n
165)Ipratropium (n 176)
? FEV1 ()
Postdose (hours)
Combivent is a registered trademark of Boehringer
Ingelheim.Bone R et al. Chest.
19941051411-1419.
48
Other Efficacy Measures Observed with Combivent

Ipratropium Albuterol Ipratropium Albuterol
Measure (n173) (n176) (n165)
CRDQ (QOL) ns ns ns
Physician Global ns ns ns Evaluation
Symptom Score ns ns ns
PEFR ns ns ns

ns not significant compared to baseline and/or
components CRDQ Chronic Respiratory Index
Questionnaire
Bone R et al. Chest. 19941051411-1419.
49
Other Efficacy Measures Observed with Serevent MDI

Rennard et al. Mahler et al.Measure
(n405) (n411)
PEF ? ?
NT Awakenings ? ?
Ventolin use ? ?
TDI (Dyspnea)
CRDQ
Diary Symptoms
Borg Dyspnea
Six min walk
COPD exac. ( pts)
Time to first exac. ?

? p0.05 salmeterol vs. placebo
pgt0.05 salmeterol vs. placebo
Am. J. Respir. Crit. Care Med.
20011631087-1092 Chest 1999115957-965.
50
Global Initiative for ChronicObstructiveLungDis
ease
Global Initiative for Chronic Obstructive Lung
Disease. Global Strategy for the Diagnosis,
Management, and Prevention of Chronic Obstructive
Pulmonary Disease NHLBI/WHO Workshop Report.
Bethesda, Md National Heart, Lung, and Blood
Institute, National Institutes of Health March
2001. NIH publication 2701A.
51
GOLD Recommendations for ICS Use
Severity
Symptoms
Spirometry
Treatment
At Risk Stage 0
/- Chronic cough, sputum
Normal
Education, avoidance risk factors, flu vaccine
Mild Stage I
FEV1 / FVC lt 70
Short-acting ?2- adrenergic PRN
/- Chronic cough, sputum
FEV1 gt 80 predicted
FEV1 / FVC lt 70 FEV1 30 - 80 predicted
Moderate Stage II A B
Reg Bronchodilator Consider ICS Rehabilitation
/- Chronic cough, sputum, dyspnea
Severe Stage III
/- Cough, sputum, dyspnea
Reg Bronchodilator Consider ICS Rehabilitation LT
Oxygen Surgery
FEV1 / FVC lt 70 FEV1 lt 30 or FEV1 lt 50 with
respiratory failure, cor pulmonale
52
A Physicians Perspective on Treatment of COPD

Smoking cessation
Bronchodilator therapy alone is not adequate in
many patients
Use of ICS in COPD

53
CONCLUSIONS

Diagnosis of COPD is based on several clinical
parameters
A large proportion of patients with COPD are
reversible
Small magnitude of response on efficacy measures
are usually observed
Guidelines support use of ICS in patients with
moderate to severe COPD

54
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55
Overview ofClinical Program

Tushar Shah, MDVice PresidentRespiratory
Clinical Development

56
Topics of Presentation

Review results of clinical program designed in
consultation with FDA
Primary objectives
FLOVENT DISKUSGreater efficacy compared to
placebo with no significant safety concerns
ADVAIR DISKUSGreater efficacy compared to
fluticasone propionate (FP) and salmeterol alone
with no significant safety concerns
Review long-term safety data with FP

57
Definitions

FSC Fluticasone propionate and Salmeterol
Combination product
FSC 500/50 ADVAIR 500
FSC 250/50 ADVAIR 250

58
Overview of Clinical Program

FLTA3025 FP 500 24 weeks
N640 FP 250
Placebo
SFCA3006 FSC 500/50 24 weeks
N691 FP 500
SAL 50
Placebo
SFCA3007 FSC 250/50 24 weeks
N723 FP 250
SAL 50
Placebo

59
Study Design FLTA3025
60
Study Design SFCA3006
FSC 500/50mcg BID (n169)
FP 500mcg BID (n173)
PRNalbuterol
SAL 50mcg BID (n164)
PlaceboRun-in
Placebo BID (n185)
2 weeks
24 weeks
61
Study Design SFCA3007
FSC 250/50mcg BID (n178)
FP 250mcg BID (n183)
PRNalbuterol
SAL 50mcg BID (n177)
PlaceboRun-in
Placebo BID (n185)
2 weeks
24 weeks
62
Key Inclusion Criteria

COPD as defined by ATS
Age ?40 years
Current or ex-smoker (?20 pack years)
Pre-bronchodilator FEV1 lt65 predicted
FEV1/FVC ?70
Dyspnea and symptoms of chronic bronchitis

63
Key Exclusion Criteria

Current diagnosis of asthma
Use of systemic corticosteroids or high dose ICS
for 6 weeks prior toscreening visit
Need for long-term oxygen therapy
COPD exacerbation during run-in

64
Primary Efficacy Measures

Pre-dose FEV1
FP vs. Placebo
FSC vs. SAL (contribution of FP)
2 hour post-dose FEV1
FSC vs. FP (contribution of SAL)

65
Secondary Efficacy Measures

Transition Dyspnea Index (TDI)
Chronic Respiratory Disease Questionnaire (CRDQ)
Chronic Bronchitis Symptoms Questionnaire (CBSQ)
Diary Card (AM PEF, Ventolin use and nighttime
awakenings)
Time to first COPD exacerbation

66
Primary Analysis

Endpoint was used to account for patient
withdrawals
Endpoint Last post-baseline observation

67
Patient Demography and Baseline Characteristics
Were Similar Across Treatment Groups

FSC250/ FSC500/
Placebo SAL50 FP250 FP500 50 50
Variable n572 n337 n399 n386 n178 n165
Age (yrs) 65 64 65 64 63 62
Gender ( male) 70 61 69 64 61 62
Race ( white) 94 94 93 94 96 95
Curr Smoker 48 49 46 47 43 46
Pack years 63 63 61 60 60 62
Prev ICS 27 25 29 28 23 28
FEV1 pred 42 41 41 41 41 41
BD resp. ( pts rev) 57 53 57 55 56 53
Emphysema 75 72 73 74 71 75

68
FLOVENTEFFICACY RESULTS
69
FLOVENT

Primary Efficacy Measure
Pre-dose FEV1
FP vs. Placebo

70
FLTA3025 Dose-Related Increases in Pre-Dose FEV1
Were Seen with FP Treatment vs. Placebo

(8)
? FEV1 (ml)
(5)
(2)
Endpoint
P0.010 vs PLA
71
SFCA3006 Significantly Greater Improvement in
Pre-Dose FEV1 Seen with FP500 vs. Placebo

(11)
? FEV1 (ml)
(2)
Endpoint
Plt0.001 vs PLA
72
SFCA3007 Significantly Greater Improvements in
Pre-Dose FEV1 Seen with FP250 vs. Placebo

(11)
? FEV1 (ml)
(1)
Endpoint
Plt0.001 vs PLA
73
SFCA3007 Additional Evidence of Improvements in
Pre-Dose FEV1 with FP250

(17)
(11)
(9)
? FEV1 (ml)
(1)
Endpoint
P0.012 vs SAL
74
Change in Pre-dose FEV1 (mL) for FP at Endpoint
in Reversible/Non-Reversible Patients
75
Greater Improvements Seen for Most Secondary
Efficacy Measures with FP vs Placebo

FLTA3025 SFCA3007 FLTA3025 SFCA3006
Measure FP250 FP250 FP500 FP500
TDI (dyspnea) ?
CRDQ (QOL) ? ?
CBSQ (cough/sputum)
PEF ? ? ? ?
NT awakenings ? ? ? ?
Ventolin use ? ? ?
Time to COPD exac.

statistically significantly different
than placebo
P0.05, FP vs. Placebo
Pgt0.05, FP vs. Placebo

76
FLOVENT EFFICACY SUMMARY

Significantly greater improvements in primary
efficacy measure (pre-dose FEV1)
Magnitude of improvement related to reversibility
Secondary efficacy measures supportive
Suggestion of dose response

77
ADVAIREFFICACY RESULTS
78
ADVAIR

Primary Efficacy Measure
Pre-dose FEV1
FSC vs. SAL (contribution of FP)

79
SFCA3006 Significantly Greater Improvement in
Pre-Dose FEV1 Seen with FSC500/50 vs. SAL50

(15)
(10)
? FEV1 (ml)
Endpoint
P0.012 vs SAL
80
SFCA3006 Significantly Greater Improvement in
Pre-Dose FEV1 Seen with FSC500/50 vs. SAL50

(15)
(11)
(10)
? FEV1 (ml)
(2)
Endpoint
P0.012 vs SAL
81
SFCA3007 Significantly Greater Improvements in
Pre-Dose FEV1 Seen with FSC250/50 vs. SAL50

(17)
(9)
? FEV1 (ml)
Endpoint
P0.012 vs SAL
82
SFCA3007 Significantly Greater Improvements in
Pre-Dose FEV1 Seen with FSC250/50 vs. SAL50

(17)
(11)
(9)
? FEV1 (ml)
(1)
Endpoint
P0.012 vs SAL
83
ADVAIR

Primary Efficacy Measure
2 hour post-dose FEV1
FSC vs. FP (contribution of SAL)

84
SFCA3006 Significantly Greater Improvements in
Post-Dose FEV1 Seen with FSC500/50 vs. FP500

(24)
(13)
? FEV1 (ml)
Endpoint
Plt0.001 vs FP
85
SFCA3006 Significantly Greater Improvements in
Post-Dose FEV1 Seen with FSC500/50 vs. FP500

(24)
(22)
(13)
? FEV1 (ml)
(4)
Endpoint
Plt0.001 vs FP
86
SFCA3007 Significantly Greater Improvements in
Post-Dose FEV1 Seen with FSC250/50 vs. FP250

(27)
(14)
? FEV1 (ml)
Endpoint
Plt0.001 vs FP
87
SFCA3007 Significantly Greater Improvements in
Post-Dose FEV1 Seen with FSC250/50 vs. FP250

(27)
(19)
(14)
? FEV1 (ml)
(6)
Endpoint
Plt0.001 vs FP
88
Change in FEV1 (mL) for FSC at Endpoint in
Reversible/Non-Reversible patients
SFCA3007
SFCA3006
PLA SAL FP FSC250/50 PLA SAL FP FSC500/50 Pre-
dose Rev. -15 141 138 196 -1 132 123 191 Non-Rev.
19 26 74 126 -8 80 93 116 2 hrPost-dose Rev. 46 2
62 179 328 29 287 161 319 Non-Rev. 71 119 107 221
28 175 111 195
89
Similar Improvements Seen in Secondary Efficacy
Measures for FP and SAL vs. PLA

SFCA3007 SFCA3007 SFCA3006 SFCA3006
Measure SAL50 FP250 SAL50 FP500
TDI (dyspnea) ?
CRDQ (QOL)
CBSQ (cough/sputum)
PEF ? ? ? ?
NT awakenings ? ? ?
Ventolin use ? ? ?
Time to COPD exac.

statistically significantly different
than placebo
P0.05, FP vs. Placebo
Pgt0.05, FP vs. Placebo

90
Greater Improvements Seen for Almost All
Secondary Efficacy Measures with FSC vs. Placebo

SFCA3007 SFCA3006
Measure FSC250/50 FSC500/50
TDI (dyspnea)
CRDQ (QOL)
CBSQ (cough/sputum)
PEF ? ?
NT awakenings ? ?
Ventolin use ? ?
Time to COPD exac

statistically significantly different
than placebo
P0.05, FP vs. Placebo
Pgt0.05, FP vs. Placebo

91
SFCA3006 Significantly Greater Improvement in
TDI Score Seen with FSC500/50 vs. SAL50 and PLA
,

TDI Score
Endpoint
P0.005 vs PLA Plt0.001 vs SAL
92
Treatment with FSC250/50 Led to Greater Increase
in AM PEF Within 1 Day
,

? PEF (L/min)

Plt0.001 vs PLA Plt0.001 FSC vs FP and SAL
93
ADVAIR EFFICACY SUMMARY

Significantly greater improvements in both trials
on the primary efficacy measures
Advair vs. salmeterol for pre-dose FEV1
Advair vs. FP for 2-hour post-dose FEV1
Magnitude of improvement related to reversibility
Secondary efficacy measures supportive
Advair 250/50 and 500/50 provide similar benefits

94
SAFETY RESULTSFlovent / Advair
95
Safety Exposure

2,054 Patients in clinical program
790 on FP
347 on Advair
Additional safety from 1298 COPD patients from
non US studiesevaluating FP
Supported by extensive safety in asthma

96
Adverse Events Occurred at Similar Frequency
Across Treatment Groups

PLA SAL50 FP250 FP500 FSC250/50
FSC500/50 n576 n341 n399 n391 n178 n169
Mean Exposure 129 139 136 132 141 138 (days)
Patients with 69 68 74 80 70 78AE ()
Patients withdrawn 6 4 6 11 5 7due to AE ()
Patients with 6 4 6 7 4 5SAE ()
Deaths 4 0 0 0 0 0

97
Similar Adverse Events of Special Interest Except
for Expected Topical Effects of ICS
PLA SAL50 FP250 FP500 FSC250/50 FSC500/50 Adver
se Events n576 n341 n399 n391 n178 n169 Can
didiasis 1 2 7 13 11 11 Throat
Irritation 6 7 9 9 8 11 Hoarseness
/ 1 lt1 5 5 5 3Dysphonia Fractures 2 lt1 1
1 2 2 Cataracts lt1 0 0 lt1 0 0 Ocular
Pressure lt1 0 0 0 0 1Disorders
98
Comparable Incidence of Pneumonia Across
Treatment Groups
PLA SAL50 FP250 FP500 FSC250/50 FSC500/50 Pneum
onia n576 n341 n399 n391 n178 n169 Adverse
Events 7 2 7 10 0 2 (1.2) (0.6)
(1.8) (2.6) (1.2) Serious Adverse 3
2 5 7 0 2Events (0.5) (0.6) (1.3)
(1.8) (1.2)
99
HPA Axis Monitoring(Performed in a Subset of
Patients)

12 hour unstimulated cortisol profile in FLTA3025
(n86)
In SFCA3006 and SFCA3007 (n359)
Morning cortisol concentrations
Short ACTH stimulation test

100
No Clinically Significant Difference in HPA Axis
Results Between FSC and Individual Agents or
Placebo

12 hour unstimulated plasma cortisol profile
FP250 10 lt placebo (N.S.)
FP500 21 lt placebo (plt0.05)
The incidence of abnormal morning cortisol was
similar across all treatment groups
The incidence of abnormal short ACTH stimulation
tests was similar across all treatment groups

101
SUMMARY OF SAFETY RESULTS

Flovent Diskus
Flovent was well tolerated
No clinically relevant safety concerns identified
compared to placebo
Advair Diskus
Advair was well tolerated
No difference in safety results between Advair
and individual agents and/or placebo

102
Long-term Safety Data with FP

Comparison of systemic exposure between patients
with asthma and COPD
Clinical studies examining bone mineral density
and ophthalmic effects in patients with asthma
Incidence of fractures and ophthalmic AEs in a 3
year clinical study in patients with COPD

103
The Range of Systemic Exposure with FP Diskus in
COPD is Not Greater Than FP CFC MDI in Asthma
Diskus 500mcg BID CFC MDI 440mcg BID
FP AUClast (pgh/mL)
Asthma
COPD
104
Clinical Studies Examining BMD and/or Ophthalmic
Effects of FP inPatients with Asthma

Two 2-year safety studies of FP vs placebo
FP 88mcg, FP 440mcg CFC MDI BID (FLTA3001)
FP 500mcg ROTADISK BID (FLTA3017)
Comparator MDI studies
FP versus BDP (3 trials)
FP versus budesonide (2 trials)

105
Mean Percent Change in Lumbar Spine BMD was
Similar Between FP Groups Compared to Placebo
Mean Percent Change from Baseline
Weeks
Data on File, GlaxoSmithKline (FLTA3001).
106
No Evidence of Cataracts orGlaucoma was Seen
with FP versus Placebo Treatment

No posterior subcapsular cataracts
No diagnosis of glaucoma

107
BMD Results from Clinical Trials Comparing FP MDI
vs. Other ICS

Treatment Groups
(mcg BID) BMD Results Reference
FP 250, 375, or 500 FP ? at all BMD sites
assessed Pauwels, 1998
versus BDP ? at femoral neck trochanter
BDP 500, 750, or 1000 Wards triangle
FP 500 versus BDP 1000 FP No vertebral
trabecular bone decline Egan, 1999
BDP ? Vertebral trabecular bone
FP and BDP ? at spine femoral neck
FP 200 versus BDP 400 FP ? at lumbar
spine Medici, 2000
FP 375 versus BDP 750 BDP ? at lumbar spine
FP 500 versus BUD 800 FP and BUD ? at lumbar
spine trochanter Hughes, 1999
FP ? at femoral neck
BUD ? at femoral neck
FP 250 versus BUD 400 FP and BUD ? at all BMD
sites assessed Harmanci, 1999

108
ISOLDE Adverse Events of Special Interest
Placebo BID FP500mcg BID n370 n372 Mean
Exposure (days) 748 824 Adverse
Events Fractures 17 (5) 9 (2) Cataracts 7
(2) 5 (1) Ocular Pressure Disorders 3
(lt1) 6 (2) Serious Adverse Events Fractures
7 (2) 4 (1)
109
SummaryLong-term Safety Data with FP

Exposure data allows extrapolation of safety data
from asthma to COPD
Two 2-year placebo controlled FP studies showed
no clinically relevant BMD or eye findings
FP vs BDP studies suggest not all ICS may have
same predisposition to effect BMD
No evidence of increased incidence of fractures
and ophthalmic AEs over 3 years of FP treatment
in COPD

110
Proposed Dosage and Administration Recommendations

For Flovent Diskus The starting dosage is 250mcg
twice daily
For Advair Diskus The starting dosage is
250/50mcg twice daily
For patients who do not respond adequately to
the starting dose, increasing the dose to 500mcg
for Flovent and 500/50 for Advair twice daily may
provide additional control.

111
CONCLUSIONS

Clinical programs achieved regulatory objectives
Flovent greater improvement in primary efficacy
measure with no safety issues
Advair superiority over individual components in
primary efficacy measures with a similar safety
profile
Long-term safety data provide further reassurance
on the use of FP in treatment of COPD

112
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113
Summary Remarks

David Wheadon, MD
Senior Vice President, Regulatory Affairs
GlaxoSmithKline

114
COPD is a Significant Public Health Problem in
the US
Proportion of 1965 Mortality Rate
3.0
Coronary Heart Disease
Stroke
Other CVD
COPD
All Other Causes
2.5
2.0
1.5
1.0
0.5
59
64
35
163
7
0
1965 - 1998
1965 - 1998
1965 - 1998
1965 - 1998
1965 - 1998
115
Current Therapeutic Managementof COPD

COPD remains under diagnosed and under treated
Bronchodilators are the only approved treatments
Additional treatment options are needed

116
Combined Effects of Salmeterol and FP in COPD
Salmeterol FP
?
Airway Obstruction
StructuralChanges
Inflammation
Increased Neutrophils,macrophages, CD8
lymphocytes. Elevated IL-8, TNFa? Protease/anti-pr
oteaseimbalance
Smooth muscle contraction Increased cholinergic
tone Loss of elastic recoil
Alveolar destruction Collagen deposition Glandular
hypertrophy Airway fibrosis