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刺猬信号通路对胰腺发育的调控

Regulation of pancreas development by hedgehog signaling.

作者信息

Hebrok M, Kim S K, St Jacques B, McMahon A P, Melton D A

机构信息

Department of Molecular and Cellular Biology and Howard Hughes Medical Institute, Harvard University, Cambridge, MA 02138, USA.

出版信息

Development. 2000 Nov;127(22):4905-13. doi: 10.1242/dev.127.22.4905.

Abstract

Pancreas organogenesis is regulated by the interaction of distinct signaling pathways that promote or restrict morphogenesis and cell differentiation. Previous work has shown that activin, a TGF(beta+) signaling molecule, permits pancreas development by repressing expression of Sonic hedgehog (Shh), a member of the hedgehog family of signaling molecules that antagonize pancreas development. Here we show that Indian hedgehog (Ihh), another hedgehog family member, and Patched 1 (Ptc1), a receptor and negative regulator of hedgehog activity, are expressed in pancreatic tissue. Targeted inactivation of Ihh in mice allows ectopic branching of ventral pancreatic tissue resulting in an annulus that encircles the duodenum, a phenotype frequently observed in humans suffering from a rare disorder known as annular pancreas. Shh(-)(/)(-) and Shh(-)(/)(-) Ihh(+/)(-) mutants have a threefold increase in pancreas mass, and a fourfold increase in pancreatic endocrine cell numbers. In contrast, mutations in Ptc1 reduce pancreas gene expression and impair glucose homeostasis. Thus, islet cell, pancreatic mass and pancreatic morphogenesis are regulated by hedgehog signaling molecules expressed within and adjacent to the embryonic pancreas. Defects in hedgehog signaling may lead to congenital pancreatic malformations and glucose intolerance.

摘要

胰腺器官发生受不同信号通路相互作用的调节,这些信号通路促进或限制形态发生和细胞分化。先前的研究表明,激活素是一种转化生长因子β(TGF-β)信号分子,它通过抑制音猬因子(Shh)的表达来促进胰腺发育,Shh是猬因子家族的信号分子成员,对胰腺发育起拮抗作用。在此我们表明,印度猬因子(Ihh)是猬因子家族的另一个成员,而patched 1(Ptc1)是猬因子活性的受体和负调节因子,它们均在胰腺组织中表达。在小鼠中对Ihh进行靶向失活会导致胰腺腹侧组织异位分支,形成环绕十二指肠的环,这种表型在患有罕见疾病环状胰腺的人类中经常观察到。Shh(-/-)和Shh(-/-)Ihh(+/-)突变体的胰腺质量增加了三倍,胰腺内分泌细胞数量增加了四倍。相反,Ptc1突变会降低胰腺基因表达并损害葡萄糖稳态。因此,胰岛细胞、胰腺质量和胰腺形态发生受胚胎胰腺内部及相邻部位表达的猬因子信号分子调节。猬因子信号缺陷可能导致先天性胰腺畸形和葡萄糖不耐受。

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