PMID- 30116539
OWN - NLM
STAT- PubMed-not-MEDLINE
LR  - 20230928
IS  - 2052-4439 (Print)
IS  - 2052-4439 (Electronic)
IS  - 2052-4439 (Linking)
VI  - 5
IP  - 1
DP  - 2018
TI  - Dose modification and dose intensity during treatment with pirfenidone: analysis 
      of pooled data from three multinational phase III trials.
PG  - e000323
LID - 10.1136/bmjresp-2018-000323 [doi]
LID - e000323
AB  - INTRODUCTION: Temporary dose modifications, such as reductions or interruptions, 
      may allow patients to better manage adverse events (AEs) associated with 
      pirfenidone use and continue treatment for idiopathic pulmonary fibrosis (IPF). 
      However, the impact of such dosing adjustments on efficacy and safety is 
      uncertain. METHODS: Patients randomised to receive treatment with pirfenidone 
      2403 mg/day or placebo in the Clinical Studies Assessing Pirfenidone in 
      Idiopathic Pulmonary Fibrosis: Research of Efficacy and Safety Outcomes (CAPACITY 
      (Study 004 (NCT00287716)) and Study 006 (NCT00287729))) and Assessment of 
      Pirfenidone to Confirm Efficacy and Safety in Idiopathic Pulmonary Fibrosis 
      (ASCEND (Study 016 (NCT01366209)) trials were included in the analysis (n=1247). 
      Descriptive statistics and a linear mixed-effects model (slope analysis) for 
      annual rate of decline in forced vital capacity (FVC) by dose intensity were 
      performed. Treatment-emergent AEs (TEAEs) were summarised and grouped by dose 
      intensity or body size. RESULTS: Dose reductions and interruptions occurred in 
      76.9% (95% CI 73.4% to 80.1%) and 46.5% (95% CI 42.6% to 50.6%) of patients 
      receiving pirfenidone vs 72.0% (95% CI 68.3% to 75.4%) and 31.1% (95% CI 27.5% to 
      34.9%) of patients receiving placebo, respectively. Dose interruptions tended to 
      occur during the first 6 months of treatment, whereas dose reductions exhibited 
      more variability. Less FVC decline from baseline was observed in patients 
      receiving pirfenidone versus placebo at >90% dose intensity (p<0.001) or 
      </=90% dose intensity (p=0.0191), showing treatment benefit in both subgroups of 
      dose intensity. No meaningful relationship between weight and TEAEs was observed. 
      CONCLUSION: Dose interruptions, which may be required to manage TEAEs, mostly 
      occurred during the first 6 months of treatment. Despite dose reductions and 
      interruptions, most patients with IPF maintained relatively high dose intensity 
      on pirfenidone, without compromising its treatment effect compared with placebo. 
      TRIAL REGISTRATION NUMBERS: NCT00287729, NCT00287716, NCT01366209.
FAU - Nathan, Steven D
AU  - Nathan SD
AD  - Inova Fairfax Hospital, Falls Church, Virginia, USA.
FAU - Lancaster, Lisa H
AU  - Lancaster LH
AD  - Vanderbilt University Medical Center, Nashville, Tennessee, USA.
FAU - Albera, Carlo
AU  - Albera C
AD  - University of Turin, Orbassano, Turin, Italy.
FAU - Glassberg, Marilyn K
AU  - Glassberg MK
AD  - Miller School of Medicine, University of Miami, Miami, Florida, USA.
FAU - Swigris, Jeffrey J
AU  - Swigris JJ
AD  - Interstitial Lung Disease Program, National Jewish Health, Denver, Colorado, USA.
FAU - Gilberg, Frank
AU  - Gilberg F
AD  - F. Hoffmann-La Roche Ltd., Basel, Switzerland.
FAU - Kirchgaessler, Klaus-Uwe
AU  - Kirchgaessler KU
AD  - F. Hoffmann-La Roche Ltd., Basel, Switzerland.
FAU - Limb, Susan L
AU  - Limb SL
AD  - Genentech, South San Francisco, California, USA.
FAU - Petzinger, Ute
AU  - Petzinger U
AD  - Accovion, Eschborn, Hessen, Germany.
FAU - Noble, Paul W
AU  - Noble PW
AD  - Cedars-Sinai Medical Center, Los Angeles, California, USA.
LA  - eng
SI  - ClinicalTrials.gov/NCT01366209
SI  - ClinicalTrials.gov/NCT00287729
SI  - ClinicalTrials.gov/NCT00287716
PT  - Journal Article
DEP - 20180802
PL  - England
TA  - BMJ Open Respir Res
JT  - BMJ open respiratory research
JID - 101638061
PMC - PMC6089326
OTO - NOTNLM
OT  - interstitial fibrosis
COIS- Competing interests: SDN was a member of the ASCEND study steering committee. He 
      has been a consultant for Genentech/Roche, served on speakers' bureaus for 
      Genentech/Roche and Boehringer Ingelheim and has received research funding from 
      Genentech/Roche and Boehringer Ingelheim. LHL was a member of the ASCEND study 
      steering committee; she has served as a consultant and on scientific advisory 
      boards for Boehringer Ingelheim, InterMune, Genentech and Veracyte. LHL has 
      participated as a clinical trial investigator for Boehringer Ingelheim, 
      Genentech, Stromedix, Gilead, Afferent, FibroGen, Bayer, Celgene and Veracyte. CA 
      was a member of the CAPACITY study steering committee; he has served on a 
      scientific advisory board for InterMune. CA has served as a consultant, steering 
      committee member and speaker for Roche, FibroGen and Boehringer Ingelheim. MKG 
      was a member of the ASCEND study steering committee. JJS was a member of the 
      ASCEND study steering committee; he has served on a scientific advisory board and 
      received research funding from InterMune. JJS served as a consultant to 
      Boehringer Ingelheim and Roche, and has received honoraria from Genentech. UP is 
      an employee of Clinipace Worldwide. PWN was a member of the ASCEND study steering 
      committee and the CAPACITY study steering committee; he has served as a 
      consultant for Boehringer Ingelheim, Bristol-Myers Squibb, InterMune, Moerae 
      Matrix, Roche and Takeda. FG and K-UK are employees of F. Hoffmann-La Roche, 
      Ltd., and K-UK is a shareholder. SLL is an employee of Genentech.
EDAT- 2018/08/18 06:00
MHDA- 2018/08/18 06:01
PMCR- 2018/08/02
CRDT- 2018/08/18 06:00
PHST- 2018/06/06 00:00 [received]
PHST- 2018/07/03 00:00 [revised]
PHST- 2018/07/06 00:00 [accepted]
PHST- 2018/08/18 06:00 [entrez]
PHST- 2018/08/18 06:00 [pubmed]
PHST- 2018/08/18 06:01 [medline]
PHST- 2018/08/02 00:00 [pmc-release]
AID - bmjresp-2018-000323 [pii]
AID - 10.1136/bmjresp-2018-000323 [doi]
PST - epublish
SO  - BMJ Open Respir Res. 2018 Aug 2;5(1):e000323. doi: 10.1136/bmjresp-2018-000323. 
      eCollection 2018.