Early Assessment of Cardiac Allograft Vasculopathy Risk Among Recipients of Hepatitis C Virus-infected Donors in the Current Era

Overview

Journal J Card Fail

Specialty Cardiology & Vascular Diseases

Date 2023 Oct 31

PMID 37907147

Authors

Kaushik Amancherla

Irene D Feurer

Scott A Rega

Andrew Cluckey

Mohamed Salih

Jonathan Davis

Dawn Pedrotty

Henry Ooi

Aniket S Rali

Hasan K Siddiqi

Jonathan Menachem

Douglas M Brinkley

Lynn Punnoose

Suzanne B Sacks

Sandip K Zalawadiya

Mark Wigger

Keki Balsara

John Trahanas

William G McMaster

Jordan Hoffman

Chetan Pasrija

JoAnn Lindenfeld

Ashish S Shah

Kelly H Schlendorf

Affiliations

Soon will be listed here.

Abstract

Background: Transplantation of hearts from hepatitis C virus (HCV)-positive donors has increased substantially in recent years following development of highly effective direct-acting antiviral therapies for treatment and cure of HCV. Although historical data from the pre-direct-acting antiviral era demonstrated an association between HCV-positive donors and accelerated cardiac allograft vasculopathy (CAV) in recipients, the relationship between the use of HCV nucleic acid test-positive (NAT+) donors and the development of CAV in the direct-acting antiviral era remains unclear.

Methods And Results: We performed a retrospective, single-center observational study comparing coronary angiographic CAV outcomes during the first year after transplant in 84 heart transplant recipients of HCV NAT+ donors and 231 recipients of HCV NAT- donors. Additionally, in a subsample of 149 patients (including 55 in the NAT+ cohort and 94 in the NAT- cohort) who had serial adjunctive intravascular ultrasound examination performed, we compared development of rapidly progressive CAV, defined as an increase in maximal intimal thickening of ≥0.5 mm in matched vessel segments during the first year post-transplant. In an unadjusted analysis, recipients of HCV NAT+ hearts had reduced survival free of CAV ≥1 over the first year after heart transplant compared with recipients of HCV NAT- hearts. After adjustment for known CAV risk factors, however, there was no significant difference between cohorts in the likelihood of the primary outcome, nor was there a difference in development of rapidly progressive CAV.

Conclusions: These findings support larger, longer-term follow-up studies to better elucidate CAV outcomes in recipients of HCV NAT+ hearts and to inform post-transplant management strategies.

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