Liver Transplantation Clinical Trial
Official title:
Pilot Study of Immunosuppression Drug Weaning in Liver Recipients Exhibiting Biomarkers of High Likelihood of Tolerance
Immunosuppressive drugs can be successfully withdrawn in a fraction of liver transplant patients. Specific peripheral blood gene expression markers can be employed to select patients with a high likelihood of being tolerant. In the current study the investigators propose to conduct a pilot non-randomized prospective study in which gradual weaning of immunosuppressive drugs will be offered to liver recipients exhibiting a favorable peripheral blood gene expression profile.
HYPOTHESIS We hypothesize that liver recipients exhibiting either specific gene expression
and/or cell phenotypic markers in peripheral blood will be successfully weaned from all
immunosuppressive drugs.
OBJECTIVE Evaluate the applicability of a set of non-invasive biomarkers in the
identification of liver transplant recipients who can successfully discontinue all
immunosuppressive therapy.
METODOLOGY
1. Immunosuppression drug weaning: according to the clinical protocol approved, all
patients will undergo liver biopsy before entry. Patients will be visited every 4
weeks, and immunosuppressive drugs will be gradually discontinued with the aim of
achieving 50% decrease in drug dosages by month 3, and complete withdrawal by month 6
after initiation of the study. Following drug discontinuation, patients will continue
to be followed every month until month 12 after initiation of the study. Liver function
tests will be obtained at every clinical follow-up visit.
2. Management of liver function test alterations: a) Increases in liver function tests
below 2-fold normal levels for AST/ALT/GGT or 1.5-fold normal levels for ALP will
result in no further decreases in drug dosages, and performance of new liver function
tests in 14 days. Worsening or persistence of liver function test alterations will
constitute indication for liver biopsy. b) Increases in liver function tests beyond
2-fold normal levels for AST/ALT/GGT or1.5-fold normal levels for ALP.
3. Diagnosis of liver graft rejection: will be based on the finding of 2 out of 3 of the
following histological criteria: portal inflammation, injury to bile duct epithelium,
and endothelitis. The finding of a mixed portal/loblular lymphocytic infiltrate not
attributable to any other cause and responding to an increase in immunosuppressive drug
doses will also be considered as a rejection.
4. Management of rejection episodes: patients presenting with mild to moderate acute
rejection will be treated with 20 mg of prednisone in decreasing doses within 4 to 6
weeks. Patients with severe acute rejection will be admitted to hospital and treated
with high dose IV prednisone (500-1000mg/day) during 3 day and thereafter oral
prednisone at decreasing dose according to evolution of liver function tests. In every
case patients will return to previous immunosuppressive dose enough to maintained
normal or near normal liver function test.
SAMPLE SIZE According to our data, the success rate of an immunosuppression withdrawal
strategy in stable liver transplant recipients transplanted for more than 3 year is 42%
(these patients are consider as operationally tolerants). Our hypothesis is that with the
use of biomarkers to identify potential tolerant patients the investigators will be able to
increase the success rate of this strategy up to 78%. In order to achieve this success rate
the sample size needed in this study is 25 patients (power 80% and significance of 95%).
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Allocation: Non-Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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