首页> 外文期刊>Journal of molecular cell biology >Zebrafish hhex-null mutant develops an intrahepatic intestinal tube due to de-repression of cdx1b and pdxl
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Zebrafish hhex-null mutant develops an intrahepatic intestinal tube due to de-repression of cdx1b and pdxl

机译:由于CDX1B和PDXL的缩小,斑马鱼HHEX-NULL突变体开发肝内肠道管

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摘要

The hepatopancreatic duct (HPD) system links the liver and pancreas to the intestinal tube and is composed of the extrahepatic biliary duct, gallbladder, and pancreatic duct. Haematopoietically expressed-homeobox (Hhex) protein plays an essential role in the establishment of HPD; however, the molecular mechanism remains elusive. Here, we show that zebrafish hhex-null mutants fail to develop the HPD system characterized by lacking the biliary marker Annexin A4 and the HPD marker sox9b. The hepatobili-ary duct part of the mutant HPD system is replaced by an intrahepatic intestinal tube characterized by expressing the intestinal marker fatty acid-binding protein 2a (fabp2a). Cell lineage analysis showed that this intrahepatic intestinal tube is not originated from hepatocytes or cholangiocytes. Further analysis revealed that cdx1b and pdx1 are expressed ectopically in the intrahepatic intestinal tube and knockdown of cdx1b and pdx1 could restore the expression of sox9b in the mutant. Chromatin-immunoprecipitation analysis showed that Hhex binds to the promoters of pdx1 and cdx1b genes to repress their expression. We therefore propose that Hhex, Cdx1b, Pdx1, and Sox9b form a genetic network governing the patterning and morphogenesis of the HPD and digestive tract systems in zebrafish.
机译:肝癌管道(HPD)系统将肝脏和胰腺链接到肠道,由肝胆管,胆囊和胰管组成。出血杂志表达 - Homeobox(HHEX)蛋白在建立HPD中起着重要作用;然而,分子机制仍然难以捉摸。在这里,我们表明斑马鱼HHEX-NULL突变体未能开发出特征的HPD系统,其特征在于缺乏胆道标记膜蛋白A4和HPD标记SOX9B。突变HPD系统的丙酸哌啶纤维导管部分由肝内肠道代替,其特征在于表达肠标记脂肪酸结合蛋白2a(Fabp2a)。细胞谱系分析表明,这种肝内肠道不源于肝细胞或胆管细胞。进一步的分析表明,CDX1B和PDX1在肝内肠道中不同地表达,CDX1b和PDX1的敲低可以恢复SOX9B在突变体中的表达。染色质 - 免疫沉淀分析表明,HHEX与PDX1和CDX1B基因的启动子结合以抑制其表达。因此,我们提出了HHEX,CDX1B,PDX1和SOX9B,形成了Zebrafish中HPD和消化道系统的图案化和形态发生的遗传网络。

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