A Modeling and Simulation-based Assessment of the Impact of Confounding Factors on the Readout of a Sildenafil Survival Trial in Pulmonary Arterial Hypertension

Overview

Journal J Pharmacokinet Pharmacodyn

Publisher Springer

Specialty Pharmacology

Date 2019 Sep 21

PMID 31538282

Citations 1

Authors

Pascal Chanu

Xiang Gao

Rene Bruno

Laurent Claret

Lutz Harnisch

Affiliations

Soon will be listed here.

Abstract

Sildenafil (REVATIO) was approved for the treatment of adult Pulmonary Arterial Hypertension (PAH) in the US and the EU. A pediatric study has been performed and sildenafil was approved in the EU for pediatric PAH. The long-term extension of this study revealed good survival but also an increased mortality with the high dose of sildenafil compared to lower doses. As a consequence, FDA required Pfizer to evaluate REVATIO's effect on the risk of death in adults with PAH. Following FDA's rationale a survival model was developed to characterize the exposure-mortality relationship and assess its potential impact on an ongoing survival trial in adults in the context of confounding factors. Clinical trial simulations were performed to assess the design of the survival trial in adults (AFFILIATE, NCT02060487), expected to last approximately 8 years according to both assumptions: absence or presence of an exposure-mortality relationship and to quantify the impact of confounding factors on its readout. Simulations showed that the trial would be robust in most conditions. But its interpretation will depend on the number of confounding factors such as additional treatments attempting to control disease progression.Clinical trial identifier NCT00159913 for STARTS-1, NCT00159874 for STARTS-2.

Citing Articles

Efficacy of Beraprost Sodium Combined with Sildenafil and Its Effects on Vascular Endothelial Function and Inflammation in Patients Experiencing Left Heart Failure Complicated with Pulmonary Arterial Hypertension.

Sun D, Yang W, Wang Z, Gao B Med Sci Monit. 2021; 27:e928413.

PMID: 33531453 PMC: 7869411. DOI: 10.12659/MSM.928413.

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