Liver Transplant; Complications Clinical Trial
Official title:
Outcome Analysis of Antiplatelet Therapy With Aspirin in Liver Transplantation
In the experimental setting inhibition of platelet activation was able to reduce
immune-mediated necroinflammatory liver disease and consecutively hepatocellular carcinoma
development. Therefore, antiplatelet therapy may not only have a preventive effect on hepatic
artery patency but also on tumor recurrence.
So far and to the best of our knowledge, no study investigated the effect of antiplatelet
therapy on hepatic arterial patency, tumor recurrence and graft survival after primary liver
transplantation.
Outcome Analysis of antiplatelet therapy with Aspirin in Liver Transplantation
BACKGROUND Arterial complications after liver transplantation (LT) are still one of the most
serious complications, which might result in liver necrosis, abscess formation, ischemic
cholangiopathy, and eventually graft loss. The sequel of these adverse events has a negative
impact on graft and patient survival and remains a life-threatening complication with a high
mortality and retransplantation rate. Therefore, an uncompromised inflow of the hepatic
artery is crucial to avoid any occlusion after LT.
In the literature, the incidence of hepatic artery thrombosis ranges between 2.5 and 10%. So
far, the possibility of preventing hepatic artery thrombosis through specific pharmacological
prophylaxis with antiplatelet agents (Aspirin) has been poorly investigated, which may be in
part due to the impaired coagulative state at the time of transplantation and the early
postoperative period. On the other hand, platelets, the chief effectors of vascular
homeostasis, have been identified as important players in the pathogenesis of both acute and
chronic liver diseases in animal models.
In the experimental setting inhibition of platelet activation was able to reduce
immune-mediated necro-inflammatory liver disease and consecutively hepatocellular carcinoma
development. Therefore, antiplatelet therapy may not only have a preventive effect on hepatic
artery patency but also on tumor recurrence.
So far and to the best of our knowledge, no study investigated the effect of antiplatelet
therapy on hepatic arterial patency, tumor recurrence and graft survival after primary liver
transplantation.
STUDY OBJECTIVES The primary goal of this study is to conduct a multicentre cohort analysis
to investigate whether antiplatelet therapy with Aspirin has an impact on hepatic arterial
patency after primary liver transplantation.
Specific aim #1: To evaluate if antiplatelet therapy with Aspirin has a protective effect on
arterial patency after primary LT.
Specific aim #2: To identify if antiplatelet therapy with Aspirin has a protective effect on
acute cellular rejection.
Specific aim #3: To identify if antiplatelet therapy with Aspirin has protective effect on
tumor recurrence (HCC).
Specific aim #4: To investigate whether antiplatelet therapy with Aspirin has a protective
effect on graft survival.
STUDY DESIGN This will be a multicentre single cohort study including only cases of deceased
donor primary liver transplantation. Primary endpoint is 30-day arterial patency in patients
with or without antiplatelet therapy with Aspirin after liver transplantation. Secondary
endpoints include postoperative complications, tumor recurrence, graft- and patient survival.
The study protocol has received approval by the local ethics committee (2016-01889) as well
as published here prior to data collection.
SETTING This multicentre cohort study will include several high-volume centres worldwide.
Each participating centre requires a prospective database from that data can be extracted.
All consecutive cases of deceased donor liver transplantation requiring from 1st of January
2013 until 31st of December 2015 are included allowing a minimum follow-up time of 24 months.
Data collection at Aspirin4olt.org will be prospective, structured, anonymized, and
encrypted.
PUBLICATION POLICY For upcoming publications, two authorships of the participating centres
will be guaranteed as a group-authorship indexed in PubMed.
INSTITUTIONAL REVIEW POLICY / ETHICAL POLICY Each participating centre is responsible to
contact their local ethics committee and receive approval for participation, if applicable.
For example, this project is considered as an audit in some countries and thus there is no
need for formal approval in the form of a protocol submission.
ELIGIBILITY CRITERIA
Inclusion criteria:
Adult Liver transplantation (age ≥18 years) Deceased donor after brain death (DBD) or
deceased donor after circulatory death (DCD) Primary liver transplantation, whole graft
Arterial anastomosis: end-to-end, back table reconstruction
Exclusion criteria:
Split liver and living donor liver transplantation Paediatric liver transplantation
(recipient age <18 years) Arterial conduits Multivisceral transplantations Retransplantations
ESTIMATED SAMPLE SIZE Each centre should provide at least 30 cases that meet the inclusion
criteria to allow adequate event rates for each outcome.
Statistical methods The primary and secondary endpoints will be compared with patient and
operation characteristics with univariate analysis. ROC Curve analysis will be performed to
dichotomize continuous variables. Multivariable analysis (binary logistic and Cox regression)
will be performed to identify independent risk factors. Statistical analysis will be
performed using R Studio version 1.0.44 (RStudio, Inc. GNU Affero General Public License v3,
Boston, MA, 2016) with the graphical user interface rBiostatistics.com beta version
(rBiostatistics.com, London, UK, 2017, GNU License).
Christian E. Oberkofler Philip C. Müller Dimitri A. Raptis Henrik Petrowsky On behalf of the
Aspirin4olt.org team Swiss HPB Center, Department of Surgery and Transplantation, University
Hospital Zurich, Switzerland
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