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通过改变表达,用果蝇直系同源物 Sox100B 替代小鼠 Sox10,为 SoxE 蛋白通过改变表达被纳入脊椎动物特异性基因调控网络的共适应提供了证据。

Replacement of mouse Sox10 by the Drosophila ortholog Sox100B provides evidence for co-option of SoxE proteins into vertebrate-specific gene-regulatory networks through altered expression.

机构信息

Institut für Biochemie, Emil-Fischer-Zentrum, Universität Erlangen, Fahrstrasse 17, D-91054 Erlangen, Germany.

出版信息

Dev Biol. 2010 May 1;341(1):267-81. doi: 10.1016/j.ydbio.2010.01.038. Epub 2010 Feb 6.

Abstract

Neural crest cells and oligodendrocytes as the myelinating glia of the central nervous system exist only in vertebrates. Their development is regulated by complex regulatory networks, of which the SoxE-type high-mobility-group domain transcription factors Sox8, Sox9 and Sox10 are essential components. Here we analyzed by in ovo electroporation in chicken and by gene replacement in the mouse whether the Drosophila ortholog Sox100B can functionally substitute for vertebrate SoxE proteins. Sox100B overexpression in the chicken neural tube led to the induction of neural crest cells as previously observed for vertebrate SoxE proteins. Furthermore, many aspects of neural crest and oligodendrocyte development were surprisingly normal in mice in which the Sox10 coding information was replaced by Sox100B arguing that Sox100B integrates well into the gene-regulatory networks that drive these processes. Our results therefore provide strong evidence for a model in which SoxE proteins were co-opted to these gene-regulatory networks mainly through the acquisition of novel expression patterns. However, later developmental defects in several neural crest derived lineages in mice homozygous for the Sox100B replacement allele indicate that some degree of functional specialization and adaptation of SoxE protein properties have taken place in addition to the co-option event.

摘要

神经嵴细胞和少突胶质细胞是中枢神经系统的髓鞘形成胶质细胞,仅存在于脊椎动物中。它们的发育受复杂的调控网络调控,其中 SoxE 型高迁移率族蛋白结构域转录因子 Sox8、Sox9 和 Sox10 是必不可少的组成部分。在这里,我们通过鸡胚电穿孔和小鼠基因替换分析了果蝇同源物 Sox100B 是否能在功能上替代脊椎动物 SoxE 蛋白。Sox100B 在鸡神经管中的过表达导致了神经嵴细胞的诱导,如先前观察到的脊椎动物 SoxE 蛋白一样。此外,在 Sox10 编码信息被 Sox100B 取代的小鼠中,神经嵴和少突胶质细胞发育的许多方面出人意料地正常,这表明 Sox100B 很好地整合到了驱动这些过程的基因调控网络中。因此,我们的研究结果为 SoxE 蛋白主要通过获得新的表达模式被共同纳入这些基因调控网络的模型提供了有力证据。然而,在 Sox100B 替代等位基因纯合的小鼠中,几个神经嵴衍生谱系的后期发育缺陷表明,除了共同纳入事件之外,SoxE 蛋白的某些功能特化和适应性也发生了。

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