Common origin and developmental dependence on c-ret of subsets of enteric and sympathetic neuroblasts.

IF 3.7 2区 生物学 Q1 DEVELOPMENTAL BIOLOGY Development Pub Date : 1996-01-01 DOI:10.1242/dev.122.1.349
P L Durbec, L B Larsson-Blomberg, A Schuchardt, F Costantini, V Pachnis
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Abstract

c-ret encodes a tyrosine kinase receptor that is necessary for normal development of the mammalian enteric nervous system. Germline mutations in c-ret lead to congenital megacolon in humans, while a loss-of-function allele (ret.k-) causes intestinal aganglionosis in mice. Here we examine in detail the function of c-ret during neurogenesis, as well as the lineage relationships among cell populations in the enteric nervous system and the sympathetic nervous system that are dependent on c-ret function. We report that, while the intestine of newborn ret.k- mice is devoid of enteric ganglia, the esophagus and stomach are only partially affected; furthermore, the superior cervical ganglion is absent, while more posterior sympathetic ganglia and the adrenal medulla are unaffected. Analysis of mutant embryos shows that the superior cervical ganglion anlage is present at E10.5, but absent by E12.5, suggesting that c-ret is required for the survival or proliferation of sympathetic neuroblasts. In situ hybridization studies, as well as direct labelling of cells with DiI, indicate that a common pool of neural crest cells derived from the postotic hindbrain normally gives rise to most of the enteric nervous system and the superior cervical ganglion, and is uniquely dependent on c-ret function for normal development. We term this the sympathoenteric lineage. In contrast, a distinct sympathoadrenal lineage derived from trunk neural crest forms the more posterior sympathetic ganglia, and also contributes to the foregut enteric nervous system. Overall, our studies reveal previously unknown complexities of cell lineage and genetic control mechanisms in the developing mammalian peripheral nervous system.

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肠和交感神经母细胞亚群c-ret的共同起源和发育依赖性。
C-ret编码酪氨酸激酶受体,酪氨酸激酶受体是哺乳动物肠神经系统正常发育所必需的。c-ret的种系突变导致人类先天性巨结肠,而功能缺失等位基因(ret.k-)导致小鼠肠神经节病。在这里,我们详细研究了c-ret在神经发生过程中的功能,以及肠神经系统和交感神经系统中依赖c-ret功能的细胞群之间的谱系关系。我们报道,虽然新生retk -小鼠的肠道缺乏肠神经节,但食管和胃仅部分受到影响;此外,颈上神经节缺失,而更多的后交感神经节和肾上腺髓质未受影响。对突变胚胎的分析表明,在E10.5时存在颈上神经节,而在E12.5时不存在,这表明c-ret是交感神经母细胞存活或增殖所必需的。原位杂交研究以及用DiI直接标记细胞表明,来自产后后脑的共同神经嵴细胞池通常会产生大部分肠神经系统和颈上神经节,并且仅依赖于c-ret功能才能正常发育。我们称之为交感肠系。相反,来自主干神经嵴的一个独特的交感肾上腺谱系形成了更后方的交感神经节,也有助于前肠肠神经系统。总的来说,我们的研究揭示了哺乳动物周围神经系统发育中未知的细胞谱系和遗传控制机制的复杂性。
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来源期刊
Development
Development 生物-发育生物学
CiteScore
6.70
自引率
4.30%
发文量
433
审稿时长
3 months
期刊介绍: Development’s scope covers all aspects of plant and animal development, including stem cell biology and regeneration. The single most important criterion for acceptance in Development is scientific excellence. Research papers (articles and reports) should therefore pose and test a significant hypothesis or address a significant question, and should provide novel perspectives that advance our understanding of development. We also encourage submission of papers that use computational methods or mathematical models to obtain significant new insights into developmental biology topics. Manuscripts that are descriptive in nature will be considered only when they lay important groundwork for a field and/or provide novel resources for understanding developmental processes of broad interest to the community. Development includes a Techniques and Resources section for the publication of new methods, datasets, and other types of resources. Papers describing new techniques should include a proof-of-principle demonstration that the technique is valuable to the developmental biology community; they need not include in-depth follow-up analysis. The technique must be described in sufficient detail to be easily replicated by other investigators. Development will also consider protocol-type papers of exceptional interest to the community. We welcome submission of Resource papers, for example those reporting new databases, systems-level datasets, or genetic resources of major value to the developmental biology community. For all papers, the data or resource described must be made available to the community with minimal restrictions upon publication. To aid navigability, Development has dedicated sections of the journal to stem cells & regeneration and to human development. The criteria for acceptance into these sections is identical to those outlined above. Authors and editors are encouraged to nominate appropriate manuscripts for inclusion in one of these sections.
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