BACKGROUND: Acute liver failure(ALF) is a serious clinical syndrome with high mortality. Sodium butyrate has been shown to alleviate organ injury in a wide variety of preclinical models of critical diseases. The aim of this study was to investigate the protective effect of sodium butyrate on ALF in rats.METHODS: All rats were randomly divided into control,model and sodium butyrate treatment groups. Except the control group, the rats were induced ALF animal model by subcutaneous injection of human serum albumin+D- galactosamine+lipopolysaccharide. After induction of ALF,the rats in the treatment group received sodium butyrate(500mg/kg) at 12-hour or 24-hour time point. Fourty-eight hours after ALF induction, the animals were sacrificed and samples were harvested. Serum endotoxin, high mobility group box-1(HMGB1), liver function parameters, tumor necrosis factoralpha(TNF-α) and interferon-gamma(IFN-γ) were measured.The expression of HMGB1 and nuclear factor-kappa B(NF-κB)p65 protein in liver tissue was detected by Western blotting. The histological changes of liver and intestine were examined. The survival duration was also observed.RESULTS: Serum endotoxin, alanine aminotransferase, HMGB1,TNF-α and IFN-γ were significantly increased and the liver histology showed more severe histopathological injury in the model group compared with the control group(P<0.05).Compared to the model group, sodium butyrate treatment significantly improved the histopathological changes in the liver and intestine, reduced serum endotoxin and inflammatory cytokines, suppressed HMGB1 and NF-кB p65 proteins in liver tissue, and prolonged the survival duration regardless of treatment at 12 hours or 24 hours after induction of ALF(P<0.05).CONCLUSIONS: Sodium butyrate protected the liver from toxin-induced ALF in rats. The mechanisms may be due to direct hepatoprotection and decreased intestinal permeability.
Fan YangLi-Kun WangXun LiLu-Wen WangXiao-Qun HanZuo-Jiong Gong
BACKGROUND:Liver failure in chronic hepatitis B(CHB) patients is a severe,life-threatening condition.Intestinal endotoxemia plays a significant role in the progress to liver failure.High mobility group box-1(HMGB1) protein is involved in the process of endotoxemia.Regulatory T(Treg) cells maintain immune tolerance and contribute to the immunological hyporesponsiveness against HBV infection.However,the roles of HMGB1 and Treg cells in the pathogenesis of liver failure in CHB patients,and whether HMGB1 affects the immune activity of Treg cells are poorly known at present,and so were explored in this study.METHODS:The levels of HMGB1 expression were detected by ELISA,real-time RT-PCR,and Western blotting,and the percentage of CD4+CD25+CD127low Treg cells among CD4+ cells was detected by flow cytometry in liver failure patients with chronic HBV infection,CHB patients,and healthy controls.Then,CD4+CD25+CD127low Treg cells isolated from the peripheral blood mononuclear cells from CHB patients were stimulated with HMGB1 at different concentrations or at various intervals.The effect of HMGB1 on the immune activity of Treg cells was assessed by a suppression assay of the allogeneic mixed lymphocyte response.The levels of forkhead box P3(Foxp3) expression in Treg cells treated with HMGB1 were detected by RT-PCR and Western blotting.RESULTS:A higher level of HMGB1 expression and a lower percentage of Treg cells within the population of CD4+ cells were found in liver failure patients than in CHB patients(82.6±20.1 μg/L vs.34.2±13.7 μg/L;4.55±1.34% vs.9.52± 3.89%,respectively).The immune activity of Treg cells was significantly weakened and the levels of Foxp3 expression were reduced in a dose-or time-dependent manner when Treg cells were stimulated with HMGB1 in vitro.CONCLUSIONS:The high level of HMGB1 and the low percentage of Treg cells play an important role in the pathogenesis of liver failure in patients with chronic HBV infection.Moreover,HMGB1 can weaken the immune activity of Treg cells.It is suggested that ef
