首页> 外文期刊>Developmental biology >pdx-1 function is specifically required in embryonic beta cells to generate appropriate numbers of endocrine cell types and maintain glucose homeostasis.
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pdx-1 function is specifically required in embryonic beta cells to generate appropriate numbers of endocrine cell types and maintain glucose homeostasis.

机译:胚胎β细胞特别需要pdx-1功能,以产生适当数量的内分泌细胞类型并维持葡萄糖稳态。

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摘要

The pdx1 gene is essential for pancreatic organogenesis in humans and mice; pdx1 mutations have been identified in human diabetic patients. Specific inactivation of pdx1 in adult beta cells revealed that this gene is required for maintenance of mature beta cell function. In the following study, a Cre-lox strategy was used to remove pdx1 function specifically from embryonic beta cells beginning at late-gestation, prior to islet formation. Animals in which pdx1 is lost in insulin-producing cells during embryogenesis had elevated blood glucose levels at birth and were overtly diabetic by weaning. Neonatal and adult mutant islets showed a dramatic reduction in the number of insulin(+) cells and an increase in both glucagon(+) and somatostatin(+) cells. Lineage tracing revealed that excess glucagon(+) and somatostatin(+) cells did not arise by interconversion of endocrine cell types. Examination of mutant islets revealed a decrease in proliferation of insulin-producing cells just before birth and a concomitant increase in proliferation of glucagon-producing cells. We propose that pdx1 is required for proliferation and function of the beta cells generated at late gestation, and that one function of normal beta cells is to inhibit the proliferation of other islet cell types, resulting in the appropriate numbers of the different endocrine cell types.
机译:pdx1基因对于人类和小鼠的胰腺器官发生至关重要。在人类糖尿病患者中已发现pdx1突变。在成年β细胞中pdx1的特定失活表明,该基因是维持成熟β细胞功能所必需的。在以下研究中,使用Cre-lox策略从妊娠后期开始的胰岛形成之前的胚胎β细胞中特异性去除pdx1功能。在胚胎发生过程中胰岛素产生细胞中丢失pdx1的动物出生时血糖水平升高,并且因断奶而明显患有糖尿病。新生儿和成年突变体胰岛显示胰岛素(+)细胞数量显着减少,胰高血糖素(+)和生长抑素(+)细胞均增加。谱系追踪显示,内分泌细胞类型的相互转化不会产生过量的胰高血糖素(+)和生长抑素(+)细胞。突变胰岛的检查显示,临产前胰岛素产生细胞的增殖减少,胰高血糖素产生细胞的增殖也随之增加。我们建议pdx1是妊娠后期生成的β细胞的增殖和功能所必需的,而正常β细胞的一种功能是抑制其他胰岛细胞类型的增殖,从而导致适当数量的不同内分泌细胞类型。

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