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Abstracts for the 11th Meeting of the International Liver Transplantation Society, July 20–23, 2005, Los Angeles, California
Author(s) -
Ng, TP,
Fan, ST,
Lam, S,
Lo, CM,
Man, K
Publication year - 2005
Publication title -
liver transplantation
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.814
H-Index - 150
eISSN - 1527-6473
pISSN - 1527-6465
DOI - 10.1002/lt.20473
Subject(s) - medicine , citation , liver transplantation , library science , transplantation , computer science
Objective
This study aims to investigate the significance of hepatic stellate cell activation at the
early phase after liver transplantation using small-for-size fatty grafts with or without
anti-inflammatory (FTY720) and/or anti-steatosis (adiponectin) therapy.
Materials and Methods
A rat orthotopic liver transplantation model using 60% of liver grafts was applied. Fatty
Zucker rats (240-280 g) with 40% liver steatosis were used as donors. Lean Zucker rats
(260-300 g) were used as recipients. Four groups of rats were included. In Group 1
(control group), no treatment was given. In Group 2 (FTY720 treatment group), FTY720
(1 mg/kg, IV) was administrated (1) at 20 minutes before graft harvesting in donors, (2)
immediately before liver out in recipients, and (3) immediately after reperfusion in
recipients. In Group 3 (adiponectin treatment group), adiponectin (1.5 mg/kg, IV) was
given at 48 and 24 hours before graft harvesting in donors, and day 1 and day 2 posttransplantation.
In Group 4 (combination therapy group), both FTY720 and adiponectin
were given. Liver tissues were sampled at 6, 24 and 48 hours after reperfusion for the
detection of hepatic stellate cell activation, intragraft protein expression of ET-1, VEGF
and RhoA. Liver function and graft survival were also compared.
Results
FTY720 or adiponectin single treatment significantly improved 7-day graft survival rate
from 0% (0/0) in the control group to 62.5% (5/8). It reached 100% (10/10) when combined
with adiponectin and FTY720. The early and significant improvement of liver function
was mainly found in the combination treatment group. Significant activation of hepatic
stellate cells, which was detected by a-SMA staining, was found in the control group at
6, 24 and 48 hours after liver transplantation. Consistently, early and overexpression of
ET-1 presented in the control group by immunostaining. Intragraft overexpression of
VEGF and RhoA was also mainly found in the control group by Western-blot. Single and
combination treatments attenuated the early activation of hepatic stellate cells
accompanied with downregulation of ET-1, VEGF and RhoA during the first 48 hours
after reperfusion.
Conclusions
Early and significant activation of hepatic stellate cells played an important role in smallfor-size
fatty liver graft injury. Combination therapy of FTY720 plus adiponectin rescued
small-for-size fatty liver grafts from injury in liver transplantation.link_to_OA_fulltex