首页> 外文期刊>Developmental dynamics: an official publication of the American Association of Anatomists >Generation and characterization of a novel neural crest marker allele, Inka1-LacZ, reveals a role for Inka1 in mouse neural tube closure.
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Generation and characterization of a novel neural crest marker allele, Inka1-LacZ, reveals a role for Inka1 in mouse neural tube closure.

机译:新型神经波峰标记等位基因Inka1-LacZ的产生和表征揭示了Inka1在小鼠神经管闭合中的作用。

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摘要

Previous studies identified Inka1 as a gene regulated by AP-2alpha in the neural crest required for craniofacial morphogenesis in fish and frog. Here, we extend the analysis of Inka1 function and regulation to the mouse by generating a LacZ knock-in allele. Inka1-LacZ allele expression occurs in the cephalic mesenchyme, heart, and paraxial mesoderm prior to E8.5. Subsequently, expression is observed in the migratory neural crest cells and their derivatives. Consistent with expression of Inka1 in tissues of the developing head during neurulation, a low percentage of Inka1(-/-) mice show exencephaly while the remainder are viable and fertile. Further studies indicate that AP-2alpha is not required for Inka1 expression in the mouse, and suggest that there is no significant genetic interaction between these two factors during embryogenesis. Together, these data demonstrate that while the expression domain of Inka1 is conserved among vertebrates, its function and regulation are not.
机译:先前的研究将Inka1确定为鱼和青蛙颅面形态发生所需的神经c中AP-2alpha调控的基因。在这里,我们通过生成LacZ敲入等位基因,将Inka1功能和调控的分析扩展到了小鼠。 Inka1-LacZ等位基因表达发生在E8.5之前的头部间质,心脏和近轴中胚层中。随后,在迁移的神经c细胞及其衍生物中观察到表达。与Inka1在发育过程中的发育中头部组织中的表达一致,低百分比的Inka1(-/-)小鼠表现出运动能力强,而其余的则具有生存能力和繁殖力。进一步的研究表明,AP-2alpha不需要在小鼠中表达Inka1,并且表明在胚胎发生过程中这两个因素之间没有显着的遗传相互作用。总之,这些数据表明,尽管Inka1的表达域在脊椎动物中是保守的,但其功能和调控却并非如此。

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