Liver Transplantation Clinical Trial
Official title:
Effect of Immunosuppression Drug Weaning on Hepatitis C Virus Induced Liver Damage After Liver Transplantation.
Viral infections can profoundly influence alloimmune responses and hamper allograft
tolerance induction. Persistent hepatitis C virus (HCV) infection occurs in 50% of liver and
20% of kidney transplant recipients, but the impact of HCV on the acquisition of allograft
tolerance has not been elucidated. Liver transplantation constitutes a unique clinical model
to address this question, given that up to 20% of liver recipients can completely
discontinue immunosuppressive drugs and attain operational tolerance.
The goal of our study is to determine the influence of HCV-driven immune responses on the
acquisition of operational tolerance in liver transplant recipients following drug weaning,
and to assess whether immunosuppression withdrawal ameliorates HCV-induced liver damage.
This is a prospective trial in which immunosuppressive drug weaning will be offered to
HCV-positive liver recipients (selected on the basis of a high likelihood of tolerance) as a
strategy to improve HCV-mediated liver disease.
Objective: To determine the influence of hepatitis C virus (HCV)-driven immune responses on
the acquisition of operational tolerance in liver transplant recipients following drug
weaning, and to assess whether immunosuppression withdrawal ameliorates HCV-induced liver
damage.
Background: Viral infections can profoundly influence alloimmune responses and hamper
allograft tolerance induction. Persistent HCV infection occurs in 50% of liver and 20% of
kidney transplant recipients, but the impact of HCV on the acquisition of allograft
tolerance has not been elucidated. Liver transplantation constitutes a unique clinical model
to address this question, given that up to 20% of liver recipients can completely
discontinue immunosuppressive drugs and attain operational tolerance.
Hypothesis/Specific Aims: We hypothesize that HCV positive patients failing to attain
operational tolerance will exhibit both decreased anti-HCV specific T cell responses and
exacerbated non-specific immunoactivation. Furthermore, we anticipate that successful
immunosuppression withdrawal will decrease the progression of HCV-induced liver damage. Thus
our aims are:
1. To test whether the magnitude of HCV-mediated inflammatory responses influence the
acquisition of operational tolerance following liver transplantation.
2. To establish the impact of anti-HCV specific CD4+ and CD8+ T cell immune responses on
the capacity of liver recipients to successfully withdraw immunosuppression.
3. To determine how the immunophenotypic traits and functional properties of T cells, NK
cells and antigen presenting cells affect the development of operational tolerance in
HCV-positive liver recipients.
4. To assess the effect of immunosuppression weaning on the histological progression of
HCV-induced liver damage.
Proposed methods: On the basis of a previously identified immunophenotypic signature of
tolerance (high ratio of delta 1 to delta 2 gammadelta T cell in peripheral blood), drug
weaning will be offered to HCV-positive liver recipients as a strategy to improve
HCV-mediated liver disease. We estimate that patients selected on the basis of this
biomarker will have a likelihood of successful weaning greater than 50%. Both peripheral
blood and liver tissue samples will be collected for diagnostic purposes before the
initiation of drug weaning in order to perform the following assays: measurement of anti-HCV
CD4+ and CD8+ T cell immunity, peripheral blood and liver tissue gene expression profiling,
peripheral blood cell phenotyping and functional assays and, in a subset of patients,
measurement of anti-donor T cell responses. Immunosuppression drugs will be weaned over a
period of 6 months, and thereafter patients will be followed for 12 additional months.
Patients not undergoing rejection during this 18 month period will be considered tolerant.
Liver biopsies will be obtained before the beginning of the study and at the end.
Progression of HCV-induced liver diseased will be compared to that of patients with a low
delta1/delta2 ratio, in whom no changes in immunosuppressive drugs will be conducted and
liver biopsies will be obtained yearly (according to our clinical guidelines).
Expected results: We expect to precisely define how HCV influences the acquisition of
operational tolerance after liver transplantation, and confirm the beneficial effect of
immunosuppression withdrawal in these patients.
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Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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