Inhaled Pulmonary Vasodilator Therapy in Adult Lung Transplant

Kamrouz Ghadimi(Duke University), Jhaymie Cappiello(Duke University), Mary Cooter-Wright(Duke University), John C. Haney(Duke University), John M. Reynolds(Duke University), Brandi Bottiger(Duke University), Jacob A. Klapper(Duke University), Jerrold H. Levy(Duke University), Matthew G. Hartwig(Duke University), INSPIRE-FLO Investigators(Inspire Institute), Angelito Agbo(Inspire Institute), Terry Ainsworth(Inspire Institute), Hakim Azfar Ali(Inspire Institute), Samuel T. Belgique(Inspire Institute), Tiffany Bisanar(Inspire Institute), Michael Blank(Inspire Institute), Desiree Bonadonna(Inspire Institute), Jason Boyle(Inspire Institute), Carla Bremenour(Inspire Institute), Jessica Burroughs(Inspire Institute), Rachel Byelene(Inspire Institute), Anne Cherry(Inspire Institute), Carl Clark(Inspire Institute), Kristen Collins(Inspire Institute), Taryn Cooper(Inspire Institute), Kelsey Decker(Inspire Institute), J Marco-del Río(Inspire Institute), Shruti Desai(Inspire Institute), Sebastian Diaz(Inspire Institute), Jill Engel(Inspire Institute), W. J. Fulkerson(Inspire Institute), Loreta Grecu(Inspire Institute), Nazish Hashmi(Inspire Institute), Teresa Hoskins(Inspire Institute), Ehimemen Iboaya(Inspire Institute), Carrie E. Johnson(Inspire Institute), Mandisa‐Maia Jones(Inspire Institute), Jörn Karhausen(Inspire Institute), Joel Kester(Inspire Institute), Rebecca Y. Klinger(Inspire Institute), Casi Larish(Inspire Institute), Trevor Lee(Inspire Institute), Jessica Lumbard(Inspire Institute), Yasmin Maisonave(Inspire Institute), Negmeldeen Mamoun(Inspire Institute), Michael W. Manning(Inspire Institute), Joseph Mathew(Inspire Institute), Sharon L. McCartney(Inspire Institute), Lynn McGugan(Inspire Institute), Beth McLendon-Arvik(Inspire Institute), Amber Mcvey(Inspire Institute), Omar Mohamedaly(Inspire Institute), Margaret A Murphy(Inspire Institute), Alina Nicoara(Inspire Institute), Thomas Owens(Inspire Institute), Scott M. Palmer(Inspire Institute), Jhana Parikh(Inspire Institute), Matthew R. Pipeling(Inspire Institute), Mihai V. Podgoreanu(Inspire Institute), Angela Pollak(Inspire Institute), Dayana Ramos(Inspire Institute), Claudette Ramsey(Inspire Institute), J. P. Ribet(Inspire Institute), Erick Saldivar(Inspire Institute), Amy Shing(Inspire Institute), Laurie D. Snyder(Inspire Institute), Kevin W. Sowers(Inspire Institute), Amanda Spiritos(Inspire Institute), Mark Stafford‐Smith(Inspire Institute), F. Gordon A. Stone(Inspire Institute), Madhav Swaminathan(Inspire Institute), Annemarie Thompson(Inspire Institute), Jamie L. Todd(Inspire Institute), Dean Van Hart(Inspire Institute), Eleanor Vega(Inspire Institute), Cameron I. Wells(Inspire Institute), Ian J. Welsby(Inspire Institute), Meredith Whitacre(Inspire Institute), Jordan Whitson(Inspire Institute), Barbara K. Wiernek(Inspire Institute), G. Wroblewski(Inspire Institute), Vincent Yeboah(Inspire Institute), Lorenzo Zaffiri(Inspire Institute)
JAMA Surgery
November 17, 2021
10.1001/jamasurg.2021.5856
Cited by 20Open Access
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Abstract

Importance: Inhaled nitric oxide (iNO) is commonly administered for selectively inhaled pulmonary vasodilation and prevention of oxidative injury after lung transplant (LT). Inhaled epoprostenol (iEPO) has been introduced worldwide as a cost-saving alternative to iNO without high-grade evidence for this indication. Objective: To investigate whether the use of iEPO will lead to similar rates of severe/grade 3 primary graft dysfunction (PGD-3) after adult LT when compared with use of iNO. Design, Setting, and Participants: This health system-funded, randomized, blinded (to participants, clinicians, data managers, and the statistician), parallel-designed, equivalence clinical trial included 201 adult patients who underwent single or bilateral LT between May 30, 2017, and March 21, 2020. Patients were grouped into 5 strata according to key prognostic clinical features and randomized per stratum to receive either iNO or iEPO at the time of LT via 1:1 treatment allocation. Interventions: Treatment with iNO or iEPO initiated in the operating room before lung allograft reperfusion and administered continously until cessation criteria met in the intensive care unit (ICU). Main Outcomes and Measures: The primary outcome was PGD-3 development at 24, 48, or 72 hours after LT. The primary analysis was for equivalence using a two one-sided test (TOST) procedure (90% CI) with a margin of 19% for between-group PGD-3 risk difference. Secondary outcomes included duration of mechanical ventilation, hospital and ICU lengths of stay, incidence and severity of acute kidney injury, postoperative tracheostomy placement, and in-hospital, 30-day, and 90-day mortality rates. An intention-to-treat analysis was performed for the primary and secondary outcomes, supplemented by per-protocol analysis for the primary outcome. Results: A total of 201 randomized patients met eligibility criteria at the time of LT (129 men [64.2%]). In the intention-to-treat population, 103 patients received iEPO and 98 received iNO. The primary outcome occurred in 46 of 103 patients (44.7%) in the iEPO group and 39 of 98 (39.8%) in the iNO group, leading to a risk difference of 4.9% (TOST 90% CI, -6.4% to 16.2%; P = .02 for equivalence). There were no significant between-group differences for secondary outcomes. Conclusions and Relevance: Among patients undergoing LT, use of iEPO was associated with similar risks for PGD-3 development and other postoperative outcomes compared with the use of iNO. Trial Registration: ClinicalTrials.gov identifier: NCT03081052.

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