Short-term outcomes of deceased donor renal transplants of HCV uninfected recipients from HCV seropositive nonviremic donors and viremic donors in the era of direct-acting antivirals

Hoz, Ricardo M. La; Sandikçi, Burhaneddi̇n; Ariyamuthu, Venkatesh Kumar; Tanrıöver, Bekir

doi:10.1111/ajt.15496

Cited by 32 publications

(23 citation statements)

References 29 publications

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“…There was no significant difference in overall graft survival or patient mortality. Further, the KDPI score was numerically lower than would historically be expected of HCV‐positive donors, which is impressive especially as HCV status is a component in the KDPI score . Similarly, the median KDPI score among patients in our series of HCV NAT (+) recipients was 52%, which was not significantly different from the median KDPI among recipients of HCV NAT (−) organs at our institution during the same time period (45%).…”

Section: Discussionmentioning

confidence: 39%

“…Even among these patients, the persistence of HCV infection post‐transplantation was associated with poor outcomes and led to worse post‐transplant survival . However, the advent of highly effective direct‐acting antiviral therapy (DAAs) has led to post‐transplantation HCV cure rates exceeding 95%, and with it, a negation of the ill effects of HCV previously seen in both LT and KT recipients . A number of clinical trials, along with data from the HCV‐TARGET cohort, have demonstrated the efficacy and safety of the use of these agents in the post‐transplant setting .…”

Section: Introductionmentioning

confidence: 99%

“…While registry data suggest excellent outcomes for HCV‐negative patients transplanted with HCV Ab (+) or ‐NAT(+) organs, there are fewer center‐level data available on this experience in LT and KT. The largest published series in LT comprised 10 patients, while in KT, the available data are predominantly from large registry data or industry‐sponsored trials, which may not always reflect the conditions of clinical practice, including the need to wait for insurance authorization before starting treatment . Therefore, this study aims to describe our experience in HCV‐positive to ‐negative organ transplantation with HCV NAT (+) donors.…”

Section: Introductionmentioning

confidence: 99%

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Liver, simultaneous liver‐kidney, and kidney transplantation from hepatitis C‐positive donors in hepatitis C‐negative recipients: A single‐center study

Crismale

Khalid

Bhansali

et al. 2019

Clinical Transplantation

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Transplantation of organs from hepatitis C virus (HCV)-antibody (Ab) and -nucleic acid test (NAT) positive donors into HCV-negative recipients has been proposed to expand the donor pool and shorten waiting times. Data on early single-center outcomes are lacking. Nineteen liver (LT, including seven simultaneous liver-kidney [SLKT]) and 17 kidney transplant (KT) recipients received organs from HCV (+) donors; of these, 13 were HCV NAT (+) in each group. All patients who received organs from HCV NAT (+) donors developed HCV viremia post-transplant except for 2 KT recipients. Patients were treated with a variety of direct-acting antiviral regimens, with high rates of sustained virologic response among those with at least 12 weeks of follow-up past the end of treatment: 12/13 (92%) and 8/8 (100%) among LT/SLKT, and KT recipients. Median time to treatment start was 42 days (interquartile range[IQR] 35-118 days) and 40 days (IQR 26-73) post-LT/SLKT and KT, respectively. One death occurred in a SLKT recipient unrelated to HCV or its treatment. There was no significant increase in rejection, proteinuria, or changes in immunosuppression in any group. Organs from HCV-viremic donors can be utilized for HCV-uninfected recipients with good short-term outcomes. K E Y W O R D Shepatitis C virus, hepatitis C-positive donors, kidney transplantation, liver transplantation 2 of 11 | CRISMALE Et AL. unacceptable due to the low efficacy and high risks associated with IFN-based therapy post-transplantation. Such organs were therefore reserved for transplantation into those already with HCV infection. Even among these patients, the persistence of HCV infection post-transplantation was associated with poor outcomes and led to worse post-transplant survival. 4,5 However, the advent of highly effective direct-acting antiviral therapy (DAAs) has led to post-transplantation HCV cure rates exceeding 95%, and with it, a negation of the ill effects of HCV previously seen in both LT and KT recipients. 6,7 A number of clinical trials, along with data from the HCV-TARGET cohort, have demonstrated the efficacy and safety of the use of these agents in the post-transplant setting. 8,9 In the HCV-TARGET cohort, adverse events leading to treatment discontinuation were uncommon, affecting only 1.6%. 8 Newer agents, including glecaprevir/ pibrentasvir (GLE/PIB), have similarly been shown to be safe and efficacious. 10 Indeed, recently published data derived from the Scientific Registry of Transplant Recipients (SRTR) suggest equivalent 1-and3-year survival among HCV-infected patients undergoing LT. 6 In the United States, the potential pool of HCV-positive organs is growing, largely due to a rising incidence of HCV in persons who inject drugs. There is significant geographic and demographic overlap between the opioid epidemic and incident HCV infection. 11 Data suggest that up to 52% of HCV-infected individuals are concentrated in 9 US states, the majority of which have a significant burden of patients suffering with opioid addiction. 12 Drug overdose...

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Section: Discussionmentioning

confidence: 39%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Liver, simultaneous liver‐kidney, and kidney transplantation from hepatitis C‐positive donors in hepatitis C‐negative recipients: A single‐center study

Crismale

Khalid

Bhansali

et al. 2019

Clinical Transplantation

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“…Single‐center studies have utilized HCV antibody positive and viremic donors for RT with good short‐term outcomes. A recent national registry analysis by our group confirms excellent short‐term outcomes for such transplants …”

Section: Introductionmentioning

confidence: 53%

“…One UNOS study of Ab+/NAT− kidneys concludes that if such kidneys are considered to be HCV‐, their survival would be comparable to the matched non‐HCV‐infected kidneys, less likely to be classified as KDPI > 85%, and the risk of DGF was significantly lower when compared to non‐HCV kidneys . A recent companion study also confirms similar or superior short‐term outcomes from transplantation with HCV+ kidneys . Hence, some authors even question the need for including HCV Ab result with donor offers and KDPI calculations and recommend uniform utilization of NAT status alone …”

Section: Discussionmentioning

confidence: 99%

Trends in utilization of deceased donor kidneys based on hepatitis C virus status and impact of public health service labeling on discard

Ariyamuthu

Sandikçi

AbdulRahim

et al. 2019

Transplant Infectious Dis

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Background Kidneys from deceased donors infected with hepatitis C virus (HCV) are underutilized. Most HCV virus‐infected donors are designated as Public Health Service increased donors (PHS‐IR). Impact of PHS and HCV designations on discard is not well studied. Methods We queried the UNOS data set for all deceased donor kidneys between January 2015 and December 2018. The final study cohort donors (n = 38 702) were stratified into three groups based on HCV antibody (Ab) and NAT status: (a) Ab−/NAT− (n = 35 861); (b) Ab+/NAT− (n = 973); and (c) Ab±/NAT+ (n = 1868). We analyzed utilization/discard rates of these organs, the impact of PHS‐IR and HCV designations on discard using multivariable two‐level hierarchical logistic regression models, forecasted number of HCV viremic donors/kidneys by 2023. Results During the study period, (a) the number of viremic donor kidneys increased 2 folds; (b) the multilevel mixed‐effects logistic regression models showed that, overall, the PHS labeling (OR 1.20, CI 95% CI 1.15‐1.29) and HCV designation (OR 2.29; 95% CI 2.15‐2.43) were independently associated with increased risk of discard; (c) contrary to the general perception, PHS‐IR kidneys across all HCV groups, compared to PHS‐IR kidneys were more likely to be discarded; (d) we forecasted that the number of kidneys from HCV viremic donor kidneys might increase from 1376 in 2019 to 2092 in 2023. Conclusion Hepatitis C virus viremic kidneys might represent 10%‐15% of deceased donor organ pool soon with the current rate of the opioid epidemic. PHS labeling effect on discard requires further discussion of the utility of this classification.

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Hepatitis C Guidance 2019 Update: American Association for the Study of Liver Diseases–Infectious Diseases Society of America Recommendations for Testing, Managing, and Treating Hepatitis C Virus Infection

2020

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Short-term outcomes of deceased donor renal transplants of HCV uninfected recipients from HCV seropositive nonviremic donors and viremic donors in the era of direct-acting antivirals

Cited by 32 publications

References 29 publications

Liver, simultaneous liver‐kidney, and kidney transplantation from hepatitis C‐positive donors in hepatitis C‐negative recipients: A single‐center study

Liver, simultaneous liver‐kidney, and kidney transplantation from hepatitis C‐positive donors in hepatitis C‐negative recipients: A single‐center study

Trends in utilization of deceased donor kidneys based on hepatitis C virus status and impact of public health service labeling on discard

Hepatitis C Guidance 2019 Update: American Association for the Study of Liver Diseases–Infectious Diseases Society of America Recommendations for Testing, Managing, and Treating Hepatitis C Virus Infection

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