Literature DB >> 16237712

Immunosuppression for liver transplantation in HCV-infected patients: mechanism-based principles.

Bijan Eghtesad1, John J Fung, Anthony J Demetris, Noriko Murase, Roberta Ness, Debra C Bass, Edward A Gray, Obaid Shakil, Bridget Flynn, Amadeo Marcos, Thomas E Starzl.   

Abstract

We retrospectively analyzed 42 hepatitis C virus (HCV)-infected patients who underwent cadaveric liver transplantation under two strategies of immunosuppression: (1) daily tacrolimus (TAC) throughout and an initial cycle of high-dose prednisone (PRED) with subsequent gradual steroid weaning, or (2) intraoperative antithymocyte globulin (ATG) and daily TAC that was later space weaned. After 36 +/- 4 months, patient and graft survival in the first group was 18/19 (94.7%) with no examples of clinically serious HCV recurrence. In the second group, the three-year patient survival was 12/23 (52%), and graft survival was 9/23 (39%); accelerated recurrent hepatitis was the principal cause of the poor results. The data were interpreted in the context of a recently proposed immunologic paradigm that is equally applicable to transplantation and viral immunity. In the framework of this paradigm, the disparate hepatitis outcomes reflected different equilibria reached under the two immunosuppression regimens between the relative kinetics of viral distribution (systemically and in the liver) and the slowly recovering HCV-specific T-cell response. As a corollary, the aims of treatment of the HCV-infected liver recipients should be to predict, monitor, and equilibrate beneficial balances between virus distribution and the absence of an immunopathologic antiviral T-cell response. In this view, favorable equilibria were accomplished in the nonweaned group of patients but not in the weaned group. In conclusion, since the anti-HCV response is unleashed when immunosuppression is weaned, treatment protocols that minimize disease recurrence in HCV-infected allograft recipients must balance the desire to reduce immunosuppression or induce allotolerance with the need to prevent antiviral immunopathology.

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Year:  2005        PMID: 16237712      PMCID: PMC2962573          DOI: 10.1002/lt.20536

Source DB:  PubMed          Journal:  Liver Transpl        ISSN: 1527-6465            Impact factor:   5.799


  39 in total

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Review 3.  Hepatitis B and hepatitis C viruses in liver transplantation.

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4.  Recurrent hepatitis C in liver allografts: prospective assessment of diagnostic accuracy, identification of pitfalls, and observations about pathogenesis.

Authors:  A J Demetris; B Eghtesad; A Marcos; K Ruppert; M A Nalesnik; P Randhawa; T Wu; A Krasinskas; P Fontes; T Cacciarelli; A O Shakil; N Murase; J J Fung; T E Starzl
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5.  Outcome of liver transplantation for hepatitis B in the United States.

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6.  Maintenance of memory CTL responses by T helper cells and CD40-CD40 ligand: antibodies provide the key.

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7.  Commentary: T cells get by with a little help from their friends.

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8.  Liver allograft. Its use in chronic active hepatitis with macronodular cirrhosis, hepatitis B surface antigen.

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Review 10.  The natural history and outcome of liver transplantation in hepatitis C virus-infected recipients.

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Review 2.  Themes of liver transplantation.

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3.  Kidney after Extrarenal Transplantation - The Impact of Alemtuzumab Induction.

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Review 4.  The unfinished legacy of liver transplantation: emphasis on immunology.

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5.  Acquired immunologic tolerance: with particular reference to transplantation.

Authors:  Thomas E Starzl
Journal:  Immunol Res       Date:  2007       Impact factor: 2.829

6.  Effect of nonviral factors on hepatitis C recurrence after liver transplantation.

Authors:  Andrew M Cameron; Rafik M Ghobrial; Jonathan R Hiatt; Ian C Carmody; Sherilyn A Gordon; Douglas G Farmer; Hasan Yersiz; Michael A Zimmerman; Francisco Durazo; Steve H Han; Sammy Saab; Jeffrey Gornbein; Ronald W Busuttil
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7.  Kidney after nonrenal transplantation-the impact of alemtuzumab induction.

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Journal:  Transplantation       Date:  2009-09-27       Impact factor: 4.939

Review 8.  Long-term management of immunosuppression after pediatric liver transplantation: is minimization or withdrawal desirable or possible or both?

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9.  Hepatitis C in Liver Allograft Recipients: Utility of One-Year Post-Transplantation Biopsy as an Indicator of Antiviral Therapy.

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