Safety and efficacy of current direct‐acting antiviral regimens in kidney and liver transplant recipients with hepatitis C: Results from the HCV‐TARGET study

Varun Saxena; Vandana Khungar; Elizabeth C. Verna; Josh Levitsky; Robert S. Brown; Mohamed A. Hassan; Mark Sulkowski; Jacqueline G. O’Leary; Farrukh M. Koraishy; Joseph Galati; Alexander Kuo; Monika Vainorius; Lucy Akushevich; David R. Nelson; Michael Fried; Norah A. Terrault; K. Rajender Reddy

doi:10.1002/hep.29258

Safety and efficacy of current direct‐acting antiviral regimens in kidney and liver transplant recipients with hepatitis C: Results from the HCV‐TARGET study

Varun Saxena(University of California, San Francisco), Vandana Khungar(University of Pennsylvania), Elizabeth C. Verna(Columbia University), Josh Levitsky(Northwestern University), Robert S. Brown(Cornell University), Mohamed A. Hassan(University of Minnesota), Mark Sulkowski(Johns Hopkins University), Jacqueline G. O’Leary(Baylor University Medical Center), Farrukh M. Koraishy(Saint Louis University), Joseph Galati(University of California, San Francisco), Alexander Kuo(University of California, San Francisco), Monika Vainorius(University of North Carolina at Chapel Hill), Lucy Akushevich(University of North Carolina at Chapel Hill), David R. Nelson(University of California, San Francisco), Michael Fried(University of North Carolina at Chapel Hill), Norah A. Terrault(University of California, San Francisco), K. Rajender Reddy(University of Pennsylvania)

Hepatology

May 15, 2017

10.1002/hep.29258

Cited by 162Open Access

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Abstract

Data outside of clinical trials with direct-acting antiviral regimens with or without ribavirin as treatment of chronic hepatitis C virus in solid organ transplant recipients are limited. Liver transplant (LT), kidney transplant (KT), and dual liver kidney (DLK) transplant recipients from the Hepatitis C Therapeutic Registry and Research Network database, a multicenter, longitudinal clinical care treatment cohort, treated with direct-acting antiviral regimens between January 1, 2014, and February 15, 2016, were included to assess safety and efficacy. Included were 443 posttransplant patients (KT = 60, LT = 347, DLK = 36); 42% had cirrhosis, and 54% had failed prior antiviral therapy. Most had genotype (GT) 1 (87% with 52% GT1a, 27% GT1b, and 8% GT1 no subtype) and were treated with sofosbuvir (SOF)/ledipasvir ± ribavirin (85%) followed by SOF + daclatasvir ± ribavirin (9%) and ombitasvir/paritaprevir/ritonavir + dasabuvir ± ribavirin (6%). Rates of sustained virologic response (SVR) at 12 weeks were available on 412 patients, and 395 patients (95.9%) achieved SVR at 12 weeks: 96.6%, 94.5%, and 90.9% among LT, KT, and DLK transplant recipients, respectively. Ribavirin did not influence SVR rates and was more often used in those with higher BMI, higher estimated glomerular filtration rate and lower creatinine. Female gender, baseline albumin ≥3.5 g/dL, baseline total bilirubin ≤1.2 mg/dL, absence of cirrhosis, and hepatic decompensation predicted SVR at 12 weeks. Six episodes of acute rejection (n = 2 KT, 4 LT) occurred, during hepatitis C virus treatment in 4 and after cessation of treatment in 2. CONCLUSION: In a large prospective observational cohort study, direct-acting antiviral therapy with SOF/ledipasvir, ombitasvir/paritaprevir/ritonavir + dasabuvir, and SOF plus daclatasvir was efficacious and safe in LT, KT, and DLK transplant recipients; ribavirin did not influence SVR, and graft rejection was rare. (Hepatology 2017;66:1090-1101).

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