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首页> 外文期刊>Gut: Journal of the British Society of Gastroenterology >Myofibroblastic cells function as progenitors to regenerate murine livers after partial hepatectomy
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Myofibroblastic cells function as progenitors to regenerate murine livers after partial hepatectomy

机译:肌纤维母细胞在部分肝切除术后可作为祖细胞再生鼠肝

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摘要

Objective Smoothened (SMO), a coreceptor of the Hedgehog (Hh) pathway, promotes fibrogenic repair of chronic liver injury. We investigated the roles of SMO+ myofibroblast (MF) in liver regeneration by conditional deletion of SMO in α smooth muscle actin (αSMA)+ cells after partial hepatectomy (PH). Design αSMA-Cre-ERT2×SMO/flox mice were treated with vehicle (VEH) or tamoxifen (TMX), and sacrificed 24-96 h post-PH. Regenerating livers were analysed for proliferation, progenitors and fibrosis by qRT-PCR and quantitative immunohistochemistry (IHC). Results were normalised to liver segments resected at PH. For lineagetracing studies, αSMA-Cre-ERT2×ROSA-Stop-flox- yellow fluorescent protein (YFP) mice were treated with VEH or TMX; livers were stained for YFP, and hepatocytes isolated 48 and 72 h post-PH were analysed for YFP by flow cytometric analysis (FACS). Results Post-PH, VEH-αSMA-SMO mice increased expression of Hh-genes, transiently accumulated MF, fibrosis and liver progenitors, and ultimately exhibited proliferation of hepatocytes and cholangiocytes. In contrast, TMX-αSMA-SMO mice showed loss of whole liver SMO expression, repression of Hh-genes, enhanced accumulation of quiescent HSC but reduced accumulation of MF, fibrosis and progenitors, as well as inhibition of hepatocyte and cholangiocyte proliferation, and reduced recovery of liver weight. In TMX-αSMA-YFP mice, many progenitors, cholangiocytes and up to 25% of hepatocytes were YFP+ by 48-72 h after PH, indicating that liver epithelial cells were derived from αSMA-YFP+ cells. Conclusions Hh signalling promotes transition of quiescent hepatic stellate cells to fibrogenic MF, some of which become progenitors that regenerate the liver epithelial compartment after PH. Hence, scarring is a component of successful liver regeneration.
机译:目标平滑化(SMO)是刺猬(Hh)途径的核心受体,可促进慢性肝损伤的纤维化修复。我们通过部分肝切除术(PH)后α平滑肌肌动蛋白(αSMA)+细胞中SMO的条件缺失,研究了SMO +肌成纤维细胞(MF)在肝脏再生中的作用。设计的αSMA-Cre-ERT2xSMO/ flox小鼠用媒介物(VEH)或他莫昔芬(TMX)处理,并在PH后24-96 h处死。通过qRT-PCR和定量免疫组织化学(IHC)分析了再生肝脏的增殖,祖细胞和纤维化。将结果标准化为在PH切除的肝段。为了进行谱系追踪研究,用VEH或TMX处理了αSMA-Cre-ERT2×ROSA-Stop-flox-黄色荧光蛋白(YFP)小鼠。对肝脏进行YFP染色,并在PH后48和72小时通过流式细胞术分析(FACS)分析分离的肝细胞的YFP。结果PH后VEH-αSMA-SMO小鼠增加Hh基因的表达,瞬时积累的MF,纤维化和肝祖细胞,并最终表现出肝细胞和胆管细胞的增殖。相反,TMX-αSMA-SMO小鼠表现出全肝SMO表达的丧失,Hh基因的抑制,静态HSC积累的增加,但MF,纤维化和祖细胞的积累减少,以及肝细胞和胆管细胞增殖的抑制,并减少肝脏重量的恢复。在TMX-αSMA-YFP小鼠中,PH后48-72 h,许多祖细胞,胆管细胞和多达25%的肝细胞为YFP +,表明肝脏上皮细胞来源于αSMA-YFP+细胞。结论Hh信号传导促进静止的肝星状细胞向纤维化MF的转化,其中一些成为PH后的肝祖细胞再生的祖细胞。因此,瘢痕形成是成功肝脏再生的组成部分。

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