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在发育中的肠道和胰腺中,Netrins和DCC对迁移的神经嵴衍生细胞的引导作用。

Netrins and DCC in the guidance of migrating neural crest-derived cells in the developing bowel and pancreas.

作者信息

Jiang Yan, Liu Min-tsai, Gershon Michael D

机构信息

Department of Anatomy and Cell Biology, Columbia University College of Physicians and Surgeons, New York, NY 10032, USA.

出版信息

Dev Biol. 2003 Jun 15;258(2):364-84. doi: 10.1016/s0012-1606(03)00136-2.

DOI:10.1016/s0012-1606(03)00136-2
PMID:12798294
Abstract

Vagal neural crest-derived precursors of the enteric nervous system colonize the bowel by descending within the enteric mesenchyme. Perpendicular secondary migration, toward the mucosa and into the pancreas, result, respectively, in the formation of submucosal and pancreatic ganglia. We tested the hypothesis that netrins guide these secondary migrations. Studies using RT-PCR, in situ hybridization, and immunocytochemistry indicated that netrins (netrins-1 and -3 mice and netrin-2 in chicks) and netrin receptors [deleted in colorectal cancer (DCC), neogenin, and the adenosine A2b receptor] are expressed by the fetal mucosal epithelium and pancreas. Crest-derived cells expressed DCC, which was developmentally regulated. Crest-derived cells migrated out of explants of gut toward cocultured cells expressing netrin-1 or toward cocultured explants of pancreas. Crest-derived cells also migrated inwardly toward the mucosa of cultured rings of bowel. These migrations were specifically blocked by antibodies to DCC and by inhibition of protein kinase A, which interferes with DCC signaling. Submucosal and pancreatic ganglia were absent at E12.5, E15, and P0 in transgenic mice lacking DCC. Netrins also promoted the survival/development of enteric crest-derived cells. The formation of submucosal and pancreatic ganglia thus involves the attraction of DCC-expressing crest-derived cells by netrins.

摘要

肠神经系统中源自迷走神经嵴的前体细胞通过在肠间充质内下行来定位于肠道。垂直的二次迁移,分别朝向黏膜和胰腺,分别导致黏膜下神经节和胰腺神经节的形成。我们测试了一种假设,即网蛋白引导这些二次迁移。使用逆转录聚合酶链反应、原位杂交和免疫细胞化学的研究表明,网蛋白(小鼠中的网蛋白-1和-3以及鸡中的网蛋白-2)和网蛋白受体(在结直肠癌中缺失的DCC、新基因和腺苷A2b受体)在胎儿黏膜上皮和胰腺中表达。源自嵴的细胞表达DCC,其表达受发育调控。源自嵴的细胞从肠道外植体迁移到共培养的表达网蛋白-1的细胞或共培养的胰腺外植体。源自嵴的细胞也向内迁移到培养的肠环黏膜。这些迁移被抗DCC抗体和干扰DCC信号传导的蛋白激酶A抑制特异性阻断。在缺乏DCC的转基因小鼠中,在胚胎第12.5天、第15天和出生后第0天没有黏膜下和胰腺神经节。网蛋白也促进了源自肠嵴的细胞的存活/发育。因此,黏膜下和胰腺神经节的形成涉及网蛋白对表达DCC的源自嵴的细胞的吸引。

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