Pulmonary Arterial Hypertension Clinical Trial
Official title:
A Randomized, Double-blind, Parallel-group, Placebo-controlled Phase 2 Trial of Ralinepag, an Oral IP Receptor Agonist, in Patients With Pulmonary Arterial Hypertension
The study was conducted as a placebo-controlled, randomized, 22-week double-blind study which included a dose titration period. An additional transition period occurred for those patients who elected to enroll into the open-label extension study, APD811-007. A total of 61 patients with PAH were enrolled.
Study APD811-003 was a 22-week, randomized, double-blind, parallel-group, placebo-controlled
study in subjects with symptomatic WHO Group 1 PAH. The study consisted of a dose titration
period of up to 9 weeks, a 13-week maintenance period, and a follow-up visit that was to
occur approximately 3 weeks after the end of the maintenance period (Week 25). The transition
period of 3 weeks (±1 week) was to occur for those subjects who elected to enroll into the
open-label extension (OLE) Study APD811-007.
Approximately 60 subjects with PAH were planned to be enrolled (61 actual). After screening,
eligible subjects were randomized 2:1 to ralinepag (APD811) or to placebo. Randomization was
stratified by baseline WHO/NYHA functional class (II versus III or IV). Subjects randomized
to active therapy were given ralinepag at a starting dose of 0.01 mg BID. Subjects randomized
to the placebo arm received matching placebo capsules to preserve the blind. Subjects were
instructed to take the study drug (ralinepag or placebo) with food. Dosage was then
uptitrated, as tolerated, over the course of the 9-week dose-titration period to a maximum
dose of 0.3 mg BID. Although doses could be reduced based on tolerability, the final dosage
reached was required to be stable during the 13-week treatment period prior to evaluation at
Week 22.
Subjects could receive concomitant oral disease-specific PAH therapy consisting of an ERA
and/or an agent acting on the nitric oxide pathway, a PDE-5 inhibitor or a sGC stimulator,
provided the dose had remained stable for at least 3 months prior to the start of screening.
It was recommended that subjects continue the same dose and regimen of these medications for
the duration of the study. With the exception of prostanoids, the use of other supporting
therapies, which may affect PAH, was also permitted.
During the study, assessments of efficacy were performed including PVR and other hemodynamic
parameters as determined by RHC, the 6MWT, assessment of clinical worsening, BNP and
NT-proBNP levels, WHO/NYHA functional class assessment of PAH. Safety assessments included
standard evaluations of AEs, clinical laboratory values, vital signs, and ECG measurements.
At the end of the maintenance period, subjects who did not choose to participate in the OLE
study were to discontinue study drug (ralinepag or placebo). All subjects that chose to
continue in the OLE study were to remain on study drug until the follow-up visit at Week 25.
This visit served as the baseline visit for the OLE study if the subject was eligible and
chose to participate.
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