TY - JOUR
T1 - Clinical trial design and new therapies for pulmonary arterial hypertension
AU - Sitbon, Olivier
AU - Gomberg-Maitland, Mardi
AU - Granton, John
AU - Lewis, Michael I.
AU - Mathai, Stephen C.
AU - Rainisio, Maurizio
AU - Stockbridge, Norman L.
AU - Wilkins, Martin R.
AU - Zamanian, Roham T.
AU - Rubin, Lewis J.
N1 - Funding Information:
Conflict of interest: O. Sitbon reports grants, personal fees and non-financial support from MSD, Actelion Pharmaceuticals and GSK, personal fees from GossamerBio, Arena Pharmaceuticals and Acceleron Pharmaceuticals, and grants and personal fees from Bayer HealthCare, outside the submitted work. M. Gomberg-Maitland is a consultant/data and safety monitoring board member/scientific advisory board member for Actelion, Acceleron, Complexa, Merck, Reata and United Therapeutics. Inova receives research support for her to do research from Actelion, AADi and United Therapeutics. J. Granton has received support from Actelion, Bayer and Pfizer to support investigator-initiated research. He is a member of a steering committee for Bellerophon clinical trial in PAH and an adjudication committee member for a clinical trial sponsored by United Therapeutics. M.I. Lewis reports that the
Funding Information:
ALPHA study cited is funded by a grant from the California Institute for Regenerative Medicine (grant CLIN2-09444). S.C. Mathai reports personal fees for consultancy and data and safety monitoring board membership from Actelion, personal fees for consultancy from United Therapeutics, and grants from Scleroderma Foundation, outside the submitted work; and is a member of the Scientific Leadership Council, Pulmonary Hypertension Association and of the Rare Disease Advisory Panel of the Patient Centered Outcomes Research Institute. M. Rainisio has nothing to disclose. N.L. Stockbridge has nothing to disclose. M.R. Wilkins reports personal fees from Actelion Pharmaceuticals, Bayer HealthCare, GossamerBio and Morphogen-IX, outside the submitted work. R.T. Zamanian is a consultant for Actelion Pharmaceuticals, Merck, Vivus and GossamerBio, and has received grants from Actelion Pharmaceuticals; and has a patent FK506, for the treatment of PAH, issued. L.J. Rubin reports personal fees from Actelion, Arena, Bellerophon, SoniVie and Roivant, during the conduct of the study.
Publisher Copyright:
Copyright © ERS 2019. This article is open access and distributed under the terms of the Creative Commons Attribution Non-Commercial Licence 4.0.
PY - 2019/1/1
Y1 - 2019/1/1
N2 - Until 20 years ago the treatment of pulmonary arterial hypertension (PAH) was based on case reports and small series, and was largely ineffectual. As a deeper understanding of the pathogenesis and pathophysiology of PAH evolved over the subsequent two decades, coupled with epidemiological studies defining the clinical and demographic characteristics of the condition, a renewed interest in treatment development emerged through collaborations between international experts, industry and regulatory agencies. These efforts led to the performance of robust, high-quality clinical trials of novel therapies that targeted putative pathogenic pathways, leading to the approval of more than 10 novel therapies that have beneficially impacted both the quality and duration of life. However, our understanding of PAH remains incomplete and there is no cure. Accordingly, efforts are now focused on identifying novel pathogenic pathways that may be targeted, and applying more rigorous clinical trial designs to better define the efficacy of these new potential treatments and their role in the management scheme. This article, prepared by a Task Force comprised of expert clinicians, trialists and regulators, summarises the current state of the art, and provides insight into the opportunities and challenges for identifying and assessing the efficacy and safety of new treatments for this challenging condition.
AB - Until 20 years ago the treatment of pulmonary arterial hypertension (PAH) was based on case reports and small series, and was largely ineffectual. As a deeper understanding of the pathogenesis and pathophysiology of PAH evolved over the subsequent two decades, coupled with epidemiological studies defining the clinical and demographic characteristics of the condition, a renewed interest in treatment development emerged through collaborations between international experts, industry and regulatory agencies. These efforts led to the performance of robust, high-quality clinical trials of novel therapies that targeted putative pathogenic pathways, leading to the approval of more than 10 novel therapies that have beneficially impacted both the quality and duration of life. However, our understanding of PAH remains incomplete and there is no cure. Accordingly, efforts are now focused on identifying novel pathogenic pathways that may be targeted, and applying more rigorous clinical trial designs to better define the efficacy of these new potential treatments and their role in the management scheme. This article, prepared by a Task Force comprised of expert clinicians, trialists and regulators, summarises the current state of the art, and provides insight into the opportunities and challenges for identifying and assessing the efficacy and safety of new treatments for this challenging condition.
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U2 - 10.1183/13993003.01908-2018
DO - 10.1183/13993003.01908-2018
M3 - Article
C2 - 30545975
AN - SCOPUS:85060534130
SN - 0903-1936
VL - 53
JO - European Respiratory Journal
JF - European Respiratory Journal
IS - 1
M1 - 1801908
ER -