TY - JOUR
T1 - Combination therapy with oral treprostinil for pulmonary arterial hypertension
T2 - A double-blind placebo-controlled clinical trial
AU - FREEDOM-EV Investigators
AU - White, R. James
AU - Jerjes-Sanchez, Carlos
AU - Meyer, Gisela Martina Bohns
AU - Pulido, Tomas
AU - Sepulveda, Pablo
AU - Wang, Kuo Yang
AU - Grünig, Ekkehard
AU - Hiremath, Shirish
AU - Yu, Zaixin
AU - Gangcheng, Zhang
AU - Yip, Wei Luen James
AU - Zhang, Shuyang
AU - Khan, Akram
AU - Deng, C. Q.
AU - Grover, Rob
AU - Tapson, Victor F.
AU - Svetliza, Noemi
AU - Lescano, Adrian Jose
AU - Bortman, Guillermo Roberto
AU - Diez, Fabian Antonio
AU - Botta, Christian Edgardo
AU - Fitzgerald, John
AU - Feenstra, Eelke
AU - Kermeen, Fiona Dawn
AU - Keogh, Anne Margaret
AU - Williams, Trevor John
AU - Yousseff, Peter Paul
AU - Ng, Benjamin Joh Han
AU - Smallwood, David Mc Naughton
AU - Dwyer, Nathan Brent
AU - Brown, Martin Russell
AU - Lang, Irene M.
AU - Steringer-Mascherbauer, Regina
AU - Arakaki, Jaquelina Ota
AU - Campos, Frederico
AU - de Amorim Correa, Ricardo
AU - de Souza, Rogerio
AU - Moreira, Maria Carmo
AU - Yoo, Hugo
AU - Lapa, Monica Silveira
AU - Swiston, John
AU - Hirani, Naushad
AU - Mehta, Sanjay
AU - Michelakis, Evangelos
AU - Zagolin, Monica
AU - Liu, Jimming
AU - Pan, Lei
AU - Chunde, Bao
AU - Segel, Michael Jonathan
AU - Ben-Dov, Issahar
N1 - Publisher Copyright:
Copyright © 2020 by the American Thoracic Society
PY - 2020/3/15
Y1 - 2020/3/15
N2 - Rationale: Oral treprostinil improves exercise capacity in patients with pulmonary arterial hypertension (PAH), but the effect on clinical outcomes was unknown. Objectives: To evaluate the effect of oral treprostinil compared with placebo on time to first adjudicated clinical worsening event in participants with PAH who recently began approved oral monotherapy. Methods: In this event-driven, double-blind study, we randomly allocated 690 participants (1:1 ratio) with PAH to receive placebo or oral treprostinil extended-release tablets three times daily. Eligible participants were using approved oral monotherapy for over 30 days before randomization and had a 6-minute-walk distance 150 m or greater. The primary endpoint was the time to first adjudicated clinical worsening event: death; hospitalization due to worsening PAH; initiation of inhaled or parenteral prostacyclin therapy; disease progression; or unsatisfactory long-term clinical response. Measurements and Main Results: Clinical worsening occurred in 26% of the oral treprostinil group compared with 36% of placebo participants (hazard ratio, 0.74; 95% confidence interval, 0.56–0.97; P = 0.028). Key measures of disease status, including functional class, Borg dyspnea score, and N-terminal pro–brain natriuretic peptide, all favored oral treprostinil treatment at Week 24 and beyond. A noninvasive risk stratification analysis demonstrated that oral treprostinil–assigned participants had a substantially higher mortality risk at baseline but achieved a lower risk profile from Study Weeks 12–60. The most common adverse events in the oral treprostinil group were headache, diarrhea, flushing, nausea, and vomiting. Conclusions: In participants with PAH, addition of oral treprostinil to approved oral monotherapy reduced the risk of clinical worsening.
AB - Rationale: Oral treprostinil improves exercise capacity in patients with pulmonary arterial hypertension (PAH), but the effect on clinical outcomes was unknown. Objectives: To evaluate the effect of oral treprostinil compared with placebo on time to first adjudicated clinical worsening event in participants with PAH who recently began approved oral monotherapy. Methods: In this event-driven, double-blind study, we randomly allocated 690 participants (1:1 ratio) with PAH to receive placebo or oral treprostinil extended-release tablets three times daily. Eligible participants were using approved oral monotherapy for over 30 days before randomization and had a 6-minute-walk distance 150 m or greater. The primary endpoint was the time to first adjudicated clinical worsening event: death; hospitalization due to worsening PAH; initiation of inhaled or parenteral prostacyclin therapy; disease progression; or unsatisfactory long-term clinical response. Measurements and Main Results: Clinical worsening occurred in 26% of the oral treprostinil group compared with 36% of placebo participants (hazard ratio, 0.74; 95% confidence interval, 0.56–0.97; P = 0.028). Key measures of disease status, including functional class, Borg dyspnea score, and N-terminal pro–brain natriuretic peptide, all favored oral treprostinil treatment at Week 24 and beyond. A noninvasive risk stratification analysis demonstrated that oral treprostinil–assigned participants had a substantially higher mortality risk at baseline but achieved a lower risk profile from Study Weeks 12–60. The most common adverse events in the oral treprostinil group were headache, diarrhea, flushing, nausea, and vomiting. Conclusions: In participants with PAH, addition of oral treprostinil to approved oral monotherapy reduced the risk of clinical worsening.
KW - Clinical study
KW - Combination therapy
KW - Oral treprostinil
KW - Pulmonary arterial hypertension
KW - Sequential therapy
UR - http://www.scopus.com/inward/record.url?scp=85081891528&partnerID=8YFLogxK
U2 - 10.1164/rccm.201908-1640OC
DO - 10.1164/rccm.201908-1640OC
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C2 - 31765604
AN - SCOPUS:85081891528
SN - 1073-449X
VL - 201
SP - 707
EP - 717
JO - American Journal of Respiratory and Critical Care Medicine
JF - American Journal of Respiratory and Critical Care Medicine
IS - 6
ER -