Objective To investigate the optimal dosage of bone marrow mesenchymal stem cells (BMSCs) transplantations for treatment of hepatic ischemia-reperfusion injury in rats, and to provide prophase experimental basis for it. Methods BMSCs of Wistar rats were isolated and cultivated by bone marrow adherent culture method. BMSCs of the fourth generation were prepared for cell transplantation. Thrity hepatic ischemia-reperfusion injury models of maleWistar rats were successfully established, and then were randomly divided into blank control group, 5×105 group, 1×106group, 2×106 group, and 3×106 group, each group enrolled 6 rats. The 200 μL cell suspension of BMSCs were transfusedinto the portal vein with number of 5×105, 1×106, 2×106, and 3×106 separately in rats of later 4 groups, and rats of blank control group were injected with phosphate buffered saline of equal volume. At 24 hours after cell transplantation, blood samples were collected to test aspartate aminotransferase (AST) and alanine aminotransferase (ALT), liver tissueswere obtained to test malonaldehyde (MDA), superoxide dismutase (SOD), and nuclear factor-κB (NF-κB) p65 protein.Liver tissues were also used to perform HE staining to observe the pathological changes. Results Compared with blank control group, 5×105 group, and 3×106 group, the levels of AST, ALT, and MDA were lower (P<0.05) while activity levels of SOD were higher (P<0.05) in 1×106 group and 2×106 group, and expression levels of NF-κB p65 protein were lower with the pathological injury of liver tissue improved, but there were no significant differences on levels of AST, ALT, MDA, and SOD (P>0.05), and both of the 2 groups had the similar pathological change. Conclusion The optimal dosage of the BMSCs transplantations after hepatic ischemia-reperfusion injury is 1×106.
ObjectiveTo investigate the effect of post-conditioning with fospropofol disodium on hepatic ischemiareperfusion (I/R) and its possible mechanism in rats. MethodsForty-eight Sprague-Dawley rats were randomly divided into four groups, including sham group (S), control group (C), propofol group (P) and fospropofol disodium group (F). According to the different periods after reperfusion, each group was further divided into 2-hour and 4-hour reperfusion subgroups respectively (n=6 in each subgroup), named S2h, C2h, P2h, and F2h subgroups and S4h, C4h, P4h, and F4h subgroups. The livers of rats were reperfused after hepatic ischemia for one hour. In the beginning of reperfusion, normal saline was infused intravenously in group S and group C continuously, propofol was infused intravenously in group P continuously, fospropofol disodium was infused continuously in group F. The blood was sampled at the end of ischemia and reperfusion for assay of alanine aminotransferase (ALT) and aspartate aminotransferase (AST). The bcl-2 and bax protein contents in liver tissue were detected by immunohistochemical analysis, and liver samples were stained with hematoxylin-eosine for histological observation and damage degree evaluation by counting the proportion of necrosis cells. ResultsThe activity of ALT and AST, the rate of necrosis cells and the amount of bcl-2 and bax protein after reperfusion in group C, group P and group F were higher than those in group S at matched reperfusion time points (P<0.05). The activity of ALT and AST, the proportion of necrosis cells and bax protein contents decreased in group P and group F, compared with group C at the same reperfusion time points, while the contents of bcl-2 protein were significantly increased (P<0.05). ConclusionFospropofol disodium can alleviate hepatic injury induced by ischemia-reperfusion in rats, in which the bcl-2 and bax protein may play important roles.