Efficacy and Safety of Selexipag in Adults With Raynaud's Phenomenon Secondary to Systemic Sclerosis:A Randomized, Placebo-Controlled, Phase II Study

6533b838fe1ef96bd12a510a

RESEARCH PRODUCT

Efficacy and Safety of Selexipag in Adults With Raynaud's Phenomenon Secondary to Systemic Sclerosis:A Randomized, Placebo-Controlled, Phase II Study

Raynaud Study Investigators Eric Hachulla Ariane L. Herrick Jean-marie R. Frenoux Christopher P. Denton Gabriela Riemekasten Aline Frey Andreas Schwarting Franck Olivier Le Brun

subject

Adult Male medicine.medical_specialty Immunology Phases of clinical research Selexipag Placebo Severity of Illness Index law.invention 03 medical and health sciences chemistry.chemical_compound 0302 clinical medicine Double-Blind Method Rheumatology Randomized controlled trial law Internal medicine Acetamides Severity of illness Clinical endpoint Humans Immunology and Allergy Medicine 030212 general & internal medicine Adverse effect Antihypertensive Agents 030203 arthritis & rheumatology Scleroderma Systemic business.industry Bayes Theorem Raynaud Disease Middle Aged Clinical trial Treatment Outcome chemistry Pyrazines Female business

description

Objective To determine the effect of selexipag, an oral, selective IP prostacyclin receptor agonist, on the frequency of attacks of Raynaud's phenomenon (RP) in patients with systemic sclerosis (SSc). Methods Patients with SSc-related RP were randomized 1:1 to placebo (n = 38) or selexipag (n = 36) in individualized doses (maximum of 1,600 μg twice daily) during a 3-week titration period. The primary end point was the weekly average number of RP attacks during the study maintenance period, analyzed using a Bayesian approach with a negative binomial model adjusted for baseline number of RP attacks. Other outcome measures included Raynaud's Condition Score (RCS), RP attack duration, and treatment-emergent adverse events (AEs). Results Baseline characteristics were comparable between treatment groups. For 83.3% of patients, the individualized maintenance dosage of selexipag was ≤800 μg twice daily. No significant difference was observed between placebo and selexipag in weekly average number of electronic diary (eDiary)–recorded RP attacks during the maintenance period (14.2 attacks during the maintenance period and 21.5 attacks during the baseline week in the placebo group [n = 32] versus 18.0 attacks during the maintenance period and 22.4 attacks during the baseline week in the selexipag group [n = 27]; adjusted mean treatment difference of 3.4 in favor of placebo). No significant treatment effect was observed on RCS or RP attack duration. In the double-blind period, 86.8% of placebo-treated patients and 100% of selexipag-treated patients reported ≥1 AE; 55.3% and 91.7%, respectively, reported ≥1 prostacyclin-associated AE. Conclusion Treatment with selexipag did not reduce the number of RP attacks compared with placebo. The safety profile of selexipag was similar to that previously reported. This study provides important information about the feasibility of eDiary reporting of RP attacks in clinical trials.

year	journal	country	edition	language
2017-11-28

10.1002/art.40242 https://doi.org/10.1002/art.40242