Direct-acting antiviral prophylaxis in kidney transplantation from hepatitis C virus-infected donors to noninfected recipients an open-label nonrandomized trial

Christine M. Durand; Mary G. Bowring; Diane M. Brown; Michael A. Chattergoon; Guido Massaccesi; Nichole Bair; Russell Wesson; Ashraf Reyad; Fizza F. Naqvi; Darin Ostrander; Jeremy Sugarman; Dorry L. Segev; Mark Sulkowski; Niraj M. Desai

doi:10.7326/M17-2871

Direct-acting antiviral prophylaxis in kidney transplantation from hepatitis C virus-infected donors to noninfected recipients an open-label nonrandomized trial

Christine M. Durand, Mary G. Bowring, Diane M. Brown, Michael A. Chattergoon, Guido Massaccesi, Nichole Bair, Russell Wesson, Ashraf Reyad, Fizza F. Naqvi, Darin Ostrander, Jeremy Sugarman, Dorry L. Segev, Mark Sulkowski, Niraj M. Desai

Research output: Contribution to journal › Article › peer-review

142 Scopus citations

Abstract

Background: Given the high mortality rate for patients with end-stage kidney disease receiving dialysis and the efficacy and safety of hepatitis C virus (HCV) treatments, discarded kidneys from HCV-infected donors may be a neglected public health resource. Objective: To determine the tolerability and feasibility of using direct-acting antivirals (DAAs) as prophylaxis before and after kidney transplantation from HCV-infected donors to non-HCV-infected recipients (that is, HCV D⁺/R transplantation). Design: Open-label nonrandomized trial. (ClinicalTrials.gov: NCT02781649) Setting: Single center. Participants: 10 HCV D⁺/R kidney transplant candidates older than 50 years with no available living donors. Intervention: Transplantation of kidneys from deceased donors aged 13 to 50 years with positive HCV RNA and HCV antibody test results. All recipients received a dose of grazoprevir (GZR), 100 mg, and elbasvir (EBR), 50 mg, immediately before transplantation. Recipients of kidneys from donors with genotype 1 infection continued receiving GZR-EBR for 12 weeks after transplantation; those receiving organs from donors with genotype 2 or 3 infection had sofosbuvir, 400 mg, added to GZR-EBR for 12 weeks of triple therapy. Measurements: The primary safety outcome was the incidence of adverse events related to GZR-EBR treatment. The primary efficacy outcome was the proportion of recipients with an HCV RNA level below the lower limit of quantification 12 weeks after prophylaxis. Results: Among 10 HCV D⁺/R transplant recipients, no treatment-related adverse events occurred, and HCV RNA was not detected in any recipient 12 weeks after treatment. Limitation: Nonrandomized study design and a small number of patients. Conclusion: Pre- and posttransplantation HCV treatment was safe and prevented chronic HCV infection in HCV D⁺/R^- kidney transplant recipients. If confirmed in larger studies, this strategy should markedly expand organ options and reduce mortality for kidney transplant candidates without HCV infection.

Original language	English (US)
Pages (from-to)	523-540
Number of pages	18
Journal	Annals of internal medicine
Volume	168
Issue number	8
DOIs	https://doi.org/10.7326/M17-2871
State	Published - Apr 17 2018

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Internal Medicine

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10.7326/M17-2871

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Durand, C. M., Bowring, M. G., Brown, D. M., Chattergoon, M. A., Massaccesi, G., Bair, N., Wesson, R., Reyad, A., Naqvi, F. F., Ostrander, D., Sugarman, J., Segev, D. L., Sulkowski, M., & Desai, N. M. (2018). Direct-acting antiviral prophylaxis in kidney transplantation from hepatitis C virus-infected donors to noninfected recipients an open-label nonrandomized trial. Annals of internal medicine, 168(8), 523-540. https://doi.org/10.7326/M17-2871

Durand, CM, Bowring, MG, Brown, DM, Chattergoon, MA, Massaccesi, G, Bair, N, Wesson, R, Reyad, A, Naqvi, FF , Ostrander, D , Sugarman, J, Segev, DL, Sulkowski, M & Desai, NM 2018, 'Direct-acting antiviral prophylaxis in kidney transplantation from hepatitis C virus-infected donors to noninfected recipients an open-label nonrandomized trial', Annals of internal medicine, vol. 168, no. 8, pp. 523-540. https://doi.org/10.7326/M17-2871

@article{7f45017fe8e542b39f1ba386059113f0,

title = "Direct-acting antiviral prophylaxis in kidney transplantation from hepatitis C virus-infected donors to noninfected recipients an open-label nonrandomized trial",

abstract = "Background: Given the high mortality rate for patients with end-stage kidney disease receiving dialysis and the efficacy and safety of hepatitis C virus (HCV) treatments, discarded kidneys from HCV-infected donors may be a neglected public health resource. Objective: To determine the tolerability and feasibility of using direct-acting antivirals (DAAs) as prophylaxis before and after kidney transplantation from HCV-infected donors to non-HCV-infected recipients (that is, HCV D+/R transplantation). Design: Open-label nonrandomized trial. (ClinicalTrials.gov: NCT02781649) Setting: Single center. Participants: 10 HCV D+/R kidney transplant candidates older than 50 years with no available living donors. Intervention: Transplantation of kidneys from deceased donors aged 13 to 50 years with positive HCV RNA and HCV antibody test results. All recipients received a dose of grazoprevir (GZR), 100 mg, and elbasvir (EBR), 50 mg, immediately before transplantation. Recipients of kidneys from donors with genotype 1 infection continued receiving GZR-EBR for 12 weeks after transplantation; those receiving organs from donors with genotype 2 or 3 infection had sofosbuvir, 400 mg, added to GZR-EBR for 12 weeks of triple therapy. Measurements: The primary safety outcome was the incidence of adverse events related to GZR-EBR treatment. The primary efficacy outcome was the proportion of recipients with an HCV RNA level below the lower limit of quantification 12 weeks after prophylaxis. Results: Among 10 HCV D+/R transplant recipients, no treatment-related adverse events occurred, and HCV RNA was not detected in any recipient 12 weeks after treatment. Limitation: Nonrandomized study design and a small number of patients. Conclusion: Pre- and posttransplantation HCV treatment was safe and prevented chronic HCV infection in HCV D+/R- kidney transplant recipients. If confirmed in larger studies, this strategy should markedly expand organ options and reduce mortality for kidney transplant candidates without HCV infection.",

author = "Durand, {Christine M.} and Bowring, {Mary G.} and Brown, {Diane M.} and Chattergoon, {Michael A.} and Guido Massaccesi and Nichole Bair and Russell Wesson and Ashraf Reyad and Naqvi, {Fizza F.} and Darin Ostrander and Jeremy Sugarman and Segev, {Dorry L.} and Mark Sulkowski and Desai, {Niraj M.}",

note = "Funding Information: Grant Support: In part, by a research grant from the Investigator-Initiated Studies Program of Merck Sharp & Dohme. Dr. Durand is supported by National Cancer Institute grant K23CA177321-01A1. Ms. Bowring is supported by National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK) grant R01AG042504 (to Dr. Segev). Dr. Segev is also supported by NIDDK grant K24DK101828. Dr. Sulkowski is supported National Institute of Allergy and Infectious Diseases grant K24DA034621. Funding Information: Disclosures: Dr. Durand reports grants from Merck Sharp & Dohme during the conduct of the study and personal fees from Merck Sharp & Dohme, Gilead Sciences, and Bristol-Myers Squibb (BMS) and grants from GlaxoSmithKline, ViiV Healthcare, Gilead Sciences, and BMS outside the submitted work. Dr. Sugarman serves on the Merck Sharp & Dohme KGaA Bioethics Advisory Panel and Stem Cell Research Oversight Committee and is a member of Quintile's Ethics Advisory Panel. Dr. Segev reports personal fees from Sanofi and No-vartis outside the submitted work. Dr. Sulkowski reports grants and personal fees from AbbVie during the conduct of the study and grants, personal fees, and research funds from Gilead; grants and personal fees from Janssen and Merck Sharp & Dohme; personal fees from Wiley and Sons and Trek; and grants from the National Institutes of Health outside the submitted work. Dr. Desai reports grants, personal fees, and nonfinancial support from Merck Sharp & Dohme during the conduct of the study. Authors not named here have disclosed no conflicts of interest. Disclosures can also be viewed at www.acponline.org/authors/icmje/ConflictOfInterestForms .do?msNum=M17-2871. Publisher Copyright: {\textcopyright} 2018 Annals of Internal Medicine. All rights reserved.",

year = "2018",

month = apr,

day = "17",

doi = "10.7326/M17-2871",

language = "English (US)",

volume = "168",

pages = "523--540",

journal = "Annals of internal medicine",

issn = "0003-4819",

publisher = "American College of Physicians",

number = "8",

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TY - JOUR

T1 - Direct-acting antiviral prophylaxis in kidney transplantation from hepatitis C virus-infected donors to noninfected recipients an open-label nonrandomized trial

AU - Durand, Christine M.

AU - Bowring, Mary G.

AU - Brown, Diane M.

AU - Chattergoon, Michael A.

AU - Massaccesi, Guido

AU - Bair, Nichole

AU - Wesson, Russell

AU - Reyad, Ashraf

AU - Naqvi, Fizza F.

AU - Ostrander, Darin

AU - Sugarman, Jeremy

AU - Segev, Dorry L.

AU - Sulkowski, Mark

AU - Desai, Niraj M.

N1 - Funding Information: Grant Support: In part, by a research grant from the Investigator-Initiated Studies Program of Merck Sharp & Dohme. Dr. Durand is supported by National Cancer Institute grant K23CA177321-01A1. Ms. Bowring is supported by National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK) grant R01AG042504 (to Dr. Segev). Dr. Segev is also supported by NIDDK grant K24DK101828. Dr. Sulkowski is supported National Institute of Allergy and Infectious Diseases grant K24DA034621. Funding Information: Disclosures: Dr. Durand reports grants from Merck Sharp & Dohme during the conduct of the study and personal fees from Merck Sharp & Dohme, Gilead Sciences, and Bristol-Myers Squibb (BMS) and grants from GlaxoSmithKline, ViiV Healthcare, Gilead Sciences, and BMS outside the submitted work. Dr. Sugarman serves on the Merck Sharp & Dohme KGaA Bioethics Advisory Panel and Stem Cell Research Oversight Committee and is a member of Quintile's Ethics Advisory Panel. Dr. Segev reports personal fees from Sanofi and No-vartis outside the submitted work. Dr. Sulkowski reports grants and personal fees from AbbVie during the conduct of the study and grants, personal fees, and research funds from Gilead; grants and personal fees from Janssen and Merck Sharp & Dohme; personal fees from Wiley and Sons and Trek; and grants from the National Institutes of Health outside the submitted work. Dr. Desai reports grants, personal fees, and nonfinancial support from Merck Sharp & Dohme during the conduct of the study. Authors not named here have disclosed no conflicts of interest. Disclosures can also be viewed at www.acponline.org/authors/icmje/ConflictOfInterestForms .do?msNum=M17-2871. Publisher Copyright: © 2018 Annals of Internal Medicine. All rights reserved.

PY - 2018/4/17

Y1 - 2018/4/17

N2 - Background: Given the high mortality rate for patients with end-stage kidney disease receiving dialysis and the efficacy and safety of hepatitis C virus (HCV) treatments, discarded kidneys from HCV-infected donors may be a neglected public health resource. Objective: To determine the tolerability and feasibility of using direct-acting antivirals (DAAs) as prophylaxis before and after kidney transplantation from HCV-infected donors to non-HCV-infected recipients (that is, HCV D+/R transplantation). Design: Open-label nonrandomized trial. (ClinicalTrials.gov: NCT02781649) Setting: Single center. Participants: 10 HCV D+/R kidney transplant candidates older than 50 years with no available living donors. Intervention: Transplantation of kidneys from deceased donors aged 13 to 50 years with positive HCV RNA and HCV antibody test results. All recipients received a dose of grazoprevir (GZR), 100 mg, and elbasvir (EBR), 50 mg, immediately before transplantation. Recipients of kidneys from donors with genotype 1 infection continued receiving GZR-EBR for 12 weeks after transplantation; those receiving organs from donors with genotype 2 or 3 infection had sofosbuvir, 400 mg, added to GZR-EBR for 12 weeks of triple therapy. Measurements: The primary safety outcome was the incidence of adverse events related to GZR-EBR treatment. The primary efficacy outcome was the proportion of recipients with an HCV RNA level below the lower limit of quantification 12 weeks after prophylaxis. Results: Among 10 HCV D+/R transplant recipients, no treatment-related adverse events occurred, and HCV RNA was not detected in any recipient 12 weeks after treatment. Limitation: Nonrandomized study design and a small number of patients. Conclusion: Pre- and posttransplantation HCV treatment was safe and prevented chronic HCV infection in HCV D+/R- kidney transplant recipients. If confirmed in larger studies, this strategy should markedly expand organ options and reduce mortality for kidney transplant candidates without HCV infection.

AB - Background: Given the high mortality rate for patients with end-stage kidney disease receiving dialysis and the efficacy and safety of hepatitis C virus (HCV) treatments, discarded kidneys from HCV-infected donors may be a neglected public health resource. Objective: To determine the tolerability and feasibility of using direct-acting antivirals (DAAs) as prophylaxis before and after kidney transplantation from HCV-infected donors to non-HCV-infected recipients (that is, HCV D+/R transplantation). Design: Open-label nonrandomized trial. (ClinicalTrials.gov: NCT02781649) Setting: Single center. Participants: 10 HCV D+/R kidney transplant candidates older than 50 years with no available living donors. Intervention: Transplantation of kidneys from deceased donors aged 13 to 50 years with positive HCV RNA and HCV antibody test results. All recipients received a dose of grazoprevir (GZR), 100 mg, and elbasvir (EBR), 50 mg, immediately before transplantation. Recipients of kidneys from donors with genotype 1 infection continued receiving GZR-EBR for 12 weeks after transplantation; those receiving organs from donors with genotype 2 or 3 infection had sofosbuvir, 400 mg, added to GZR-EBR for 12 weeks of triple therapy. Measurements: The primary safety outcome was the incidence of adverse events related to GZR-EBR treatment. The primary efficacy outcome was the proportion of recipients with an HCV RNA level below the lower limit of quantification 12 weeks after prophylaxis. Results: Among 10 HCV D+/R transplant recipients, no treatment-related adverse events occurred, and HCV RNA was not detected in any recipient 12 weeks after treatment. Limitation: Nonrandomized study design and a small number of patients. Conclusion: Pre- and posttransplantation HCV treatment was safe and prevented chronic HCV infection in HCV D+/R- kidney transplant recipients. If confirmed in larger studies, this strategy should markedly expand organ options and reduce mortality for kidney transplant candidates without HCV infection.

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Direct-acting antiviral prophylaxis in kidney transplantation from hepatitis C virus-infected donors to noninfected recipients an open-label nonrandomized trial

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