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Combined obeticholic acid and apoptosis inhibitor treatment alleviates liver fibrosis 被引量:15
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作者 Jiyu Zhou Ningning Huang +7 位作者 Yitong Guo Shuang Cui Chaoliang Ge qingxian he Xiaojie Pan Guangji Wang Hong Wang Haiping Hao 《Acta Pharmaceutica Sinica B》 SCIE CAS CSCD 2019年第3期526-536,共11页
Obeticholic acid(OCA), the first FXR-targeting drug, has been claimed effective in the therapy of liver fibrosis. However, recent clinical trials indicated that OCA might not be effective against liver fibrosis, possi... Obeticholic acid(OCA), the first FXR-targeting drug, has been claimed effective in the therapy of liver fibrosis. However, recent clinical trials indicated that OCA might not be effective against liver fibrosis, possibly due to the lower dosage to reduce the incidence of the side-effect of pruritus. Here we propose a combinatory therapeutic strategy of OCA and apoptosis inhibitor for combating against liver fibrosis. CCl4-injured mice, D-galactosamine/LPS(GalN/LPS)-treated mice and cycloheximide/TNFα(CHX/TNFα)-treated HepG2 cells were employed to assess the effects of OCA, or together with IDN-6556, an apoptosis inhibitor. OCA treatment significantly inhibited hepatic stellate cell(HSC)activation/proliferation and prevented fibrosis. Elevated bile acid(BA) levels and hepatocyte apoptosis triggered the activation and proliferation of HSCs. OCA treatment reduced BA levels but could not inhibit hepatocellular apoptosis. An enhanced anti-fibrotic effect was observed when OCA was co-administrated with IDN-6556. Our study demonstrated that OCA inhibits HSCs activation/proliferation partially by regulating BA homeostasis and thereby inhibiting activation of HSCs. The findings in this study suggest that combined use of apoptosis inhibitor and OCA at lower dosage represents a novel therapeutic strategy for liver fibrosis. 展开更多
关键词 Obeticholic ACID Liver FIBROSIS BILE ACID HEPATOCELLULAR APOPTOSIS IDN-6556 Farnesoid X receptor Hepatic stellate cell
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