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神经嵴发出的信号调节胰腺中的β细胞数量。

Signals from the neural crest regulate beta-cell mass in the pancreas.

作者信息

Nekrep Nada, Wang Juehu, Miyatsuka Takeshi, German Michael S

机构信息

Diabetes Center, Hormone Research Institute, University of California at San Francisco, San Francisco, CA 94143, USA.

出版信息

Development. 2008 Jun;135(12):2151-60. doi: 10.1242/dev.015859.

DOI:10.1242/dev.015859
PMID:18506029
Abstract

Pancreatic islet cells and neurons share common functions and similar ontogenies, but originate in different germ layers. To determine whether ectoderm-derived cells contribute instructive signals to the developing endoderm-derived pancreas, we defined the chronology of migration and differentiation of neural crest cells in the pancreas, and tested their role in the development of the islets. The homeodomain transcription factor Phox2b marks the neural precursors from the neural crest that colonize the gut to form the enteric nervous system. In the embryonic mouse pancreas, we found Phox2b expressed briefly together with Sox10 along the epithelial-mesenchymal border at E12.5 in cells derived from the neural crest. Downregulation of Phox2b shortly thereafter was dependent upon Nkx2.2 expressed in the adjacent pancreatic epithelium. In Phox2b(-/-) embryos, neurons and glia did not develop in the pancreas, and Nkx2.2 expression was markedly upregulated in the epithelium. In addition, the number and replication rate of insulin-expressing beta-cells increased in the Phox2b(-/-) mice. We conclude that, during pancreatic development, Phox2b and Nkx2.2 form a non-cell-autonomous feedback loop that links the neural crest with the pancreatic epithelium, regulates the size of the beta-cell population, and thereby impacts insulin-secretory capacity and energy homeostasis.

摘要

胰岛细胞和神经元具有共同的功能和相似的个体发生过程,但起源于不同的胚层。为了确定外胚层来源的细胞是否为发育中的内胚层来源的胰腺提供指导性信号,我们确定了胰腺中神经嵴细胞迁移和分化的时间顺序,并测试了它们在胰岛发育中的作用。同源结构域转录因子Phox2b标记来自神经嵴的神经前体细胞,这些细胞定殖于肠道以形成肠神经系统。在胚胎小鼠胰腺中,我们发现Phox2b在E12.5时与Sox10一起在神经嵴来源的细胞中沿上皮-间充质边界短暂表达。此后不久Phox2b的下调依赖于相邻胰腺上皮中表达的Nkx2.2。在Phox2b基因敲除(-/-)胚胎中,胰腺中神经元和神经胶质细胞未发育,上皮中Nkx2.2表达明显上调。此外,Phox2b基因敲除(-/-)小鼠中表达胰岛素的β细胞数量和复制率增加。我们得出结论,在胰腺发育过程中,Phox2b和Nkx2.2形成一个非细胞自主反馈环,将神经嵴与胰腺上皮联系起来,调节β细胞群体的大小,从而影响胰岛素分泌能力和能量稳态。

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