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Arx is required for normal enteroendocrine cell development in mice and humans

机译:小鼠和人类正常肠内分泌细胞发育需要Arx

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Enteroendocrine cells of the gastrointestinal (GI) tract play a central role in metabolism, digestion, satiety and lipid absorption, yet their development remains poorly understood. Here we show that Arx, a homeodomain-containing transcription factor, is required for the normal development of mouse and human enteroendocrine cells. Arx expression is detected in a subset of Neurogenin3 (Ngn3)-positive endocrine progenitors and is also found in a subset of hormone-producing cells. In mice, removal of Arx from the developing endoderm results in a decrease of enteroendocrine cell types including gastrin-, glucagon/GLP-1-, CCK-, secretin-producing cell populations and an increase of somatostatin-expressing cells. This phenotype is also observed in mice with endocrine-progenitor-specific Arx ablation suggesting that Arx is required in the progenitor for enteroendocrine cell development. In addition, depletion of human ARX in developing human intestinal tissue results in a profound deficit in expression of the enteroendocrine cell markers CCK, secretin and glucagon while expression of a pan-intestinal epithelial marker, CDX2, and other non-endocrine markers remained unchanged. Taken together, our findings uncover a novel and conserved role of Arx in mammalian endocrine cell development and provide a potential cause for the chronic diarrhea seen in both humans and mice carrying Arx mutations.
机译:胃肠道(GI)的肠内分泌细胞在新陈代谢,消化,饱腹感和脂质吸收中起着核心作用,但其发展仍知之甚少。在这里,我们显示Arx,一种含同源结构域的转录因子,是小鼠和人类肠内分泌细胞正常发育所必需的。在Neurogenin3(Ngn3)阳性内分泌祖细胞的一个子集中检测到Arx表达,并且在一个激素生成细胞的子集中也发现了Arx表达。在小鼠中,从发育中的内胚层中去除Arx会导致肠内分泌细胞类型的减少,包括胃泌素,胰高血糖素/ GLP-1,CCK,产生促胰液素的细胞群,以及生长抑素表达细胞的增加。在具有内分泌祖细胞特异性Arx消融的小鼠中也观察到该表型,这表明在祖细胞中肠内分泌细胞发育需要Arx。另外,在发育中的人肠组织中人ARX的消耗导致肠内分泌细胞标志物CCK,促胰液素和胰高血糖素的表达严重不足,而全肠上皮标志物,CDX2和其他非内分泌标志物的表达保持不变。综上所述,我们的发现揭示了Arx在哺乳动物内分泌细胞发育中的新颖且保守的作用,并为人类和携带Arx突变的小鼠中出现的慢性腹泻提供了潜在的原因。

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