Using HCV-viremic organs for lung transplantation does not confer higher rejection rates compared to HCV-negative organs

Kamyar Afshar; Elizabeth Schonhoft; Jade Kozuch; Aarya Kafi; Gordon Yung; Travis Pollema; Eugene Golts; Saima Aslam

doi:10.1111/ctr.15260

Using HCV-viremic organs for lung transplantation does not confer higher rejection rates compared to HCV-negative organs

Clin Transplant. 2024 Feb;38(2):e15260. doi: 10.1111/ctr.15260.

Authors

Kamyar Afshar¹, Elizabeth Schonhoft¹, Jade Kozuch¹, Aarya Kafi¹, Gordon Yung¹, Travis Pollema¹, Eugene Golts¹, Saima Aslam¹

Affiliation

¹ Clinical Professor of Medicine, Medical Director, UC San Diego Lung Transplant Program, La Jolla, USA.

PMID: 38369851
DOI: 10.1111/ctr.15260

Abstract

Background: National data demonstrate that hepatitis C virus (HCV)-infected organ donors are increasingly being used in the US, including for lung transplantation. We aimed to assess whether there were any differences in the acute or chronic rejection rates at 1 year following lung transplantation from HCV-viremic versus uninfected donors.

Methods: We retrospectively reviewed all lung transplant recipients at our institution from April 1, 2017 to October 1, 2020 and then assessed various outcomes between those who received a transplant from HCV-viremic donors versus HCV-negative donors. Primary outcome was to determine if there was a higher incidence of acute and/or chronic allograft rejection when using HCV NAT+ lung donation. We carried out univariate and multivariate analyses.

Results: We transplanted 135 patients during the study period, including 18 from HCV-viremic donors. Standard induction therapy with basiliximab and maintenance triple drug immunosuppression was utilized per UC San Diego protocol. All 17 patients receiving HCV-viremic organs developed acute HCV infection and were treated in the postoperative period with 12 weeks of direct acting antivirals (DAA). HCV genotypes included 1, 2, and 3. DAA used included glecaprevir/pibrentasvir (12), sofosbuvir/velpatasvir (1), and ledipasvir/sofosbuvir (2) with drug choice determined by patient's medical insurance coverage. Sustained virological response at 12 weeks after end of DAA therapy (SVR12), indicative of a cure, was achieved in all (100%) recipients. No recipient had a serious adverse event related to HCV infection. The lung transplant recipient (LTR) HCV-viremic donors had lower rates of clinically significant rejection (5.9% vs. 11% LTR HCV-nonviremic donors), and no chronic lung allograft dysfunction at 1 year (vs. 5.9% LTR HCV-nonviremic donors). One-year survival was 100% in the LTR HCV-viremic donors compared to 95.8% in the LTR HCV-nonviremic donors.

Conclusions: We demonstrate the feasibility and success of using HCV NAT + donors with excellent results and without a higher incidence of rejection. Longer term follow-up and a larger sample size are needed to allow this to be a more widely accepted practice for lung transplant programs and payors.

Keywords: donor-derived infections; donors and donation; infection and infectious agents; lung (allograft) function/dysfunction.

MeSH terms

Antiviral Agents / therapeutic use
Hepacivirus
Hepatitis C* / drug therapy
Hepatitis C, Chronic*
Humans
Lung Transplantation*
Retrospective Studies
Sofosbuvir / therapeutic use
Tissue Donors

Substances

Sofosbuvir
Antiviral Agents