首页> 外文OA文献 >Caenorhabditis elegans WASP and Ena/VASP proteins play compensatory roles in morphogenesis and neuronal cell migration.
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Caenorhabditis elegans WASP and Ena/VASP proteins play compensatory roles in morphogenesis and neuronal cell migration.

机译:秀丽隐杆线虫WASP和Ena / VASP蛋白在形态发生和神经元细胞迁移中起补偿作用。

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摘要

We report here that WASP and Ena/VASP family proteins play overlapping roles in C. elegans morphogenesis and neuronal cell migration. Specifically, these studies demonstrate that UNC-34/Ena plays a role in morphogenesis that is revealed only in the absence of WSP-1 function and that WSP-1 has a role in neuronal cell migration that is revealed only in the absence of UNC-34/Ena activity. To identify additional genes that act in parallel to unc-34/ena during morphogenesis, we performed a screen for synthetic lethals in an unc-34 null mutant background utilizing an RNAi feeding approach. To our knowledge, this is the first reported RNAi-based screen for genetic interactors. As a result of this screen, we identified a second C. elegans WASP family protein, wve-1, that is most homologous to SCAR/WAVE proteins. Animals with impaired wve-1 function display defects in gastrulation, fail to undergo proper morphogenesis, and exhibit defects in neuronal cell migrations and axon outgrowth. Reducing wve-1 levels in either unc-34/ena or wsp-1 mutant backgrounds also leads to a significant enhancement of the gastrulation and morphogenesis defects. Thus, unc-34/ena, wsp-1, and wve-1 play overlapping roles during embryogenesis and unc-34/ena and wsp-1 play overlapping roles in neuronal cell migration. These observations show that WASP and Ena/VASP proteins can compensate for each other in vivo and provide the first demonstration of a role for Ena/VASP proteins in gastrulation and morphogenesis. In addition, our results provide the first example of an in vivo role for WASP family proteins in neuronal cell migrations and cytokinesis in metazoans.
机译:我们在这里报告WASP和Ena / VASP家族蛋白在秀丽隐杆线虫形态发生和神经元细胞迁移中起重叠作用。具体而言,这些研究表明UNC-34 / Ena在形态发生中起作用,仅在没有WSP-1功能的情况下才显示,而WSP-1在神经元细胞迁移中的作用仅在没有UNC-34的情况下才显示。 34 / Ena活动。为了鉴定在形态发生过程中与unc-34 / ena平行发挥作用的其他基因,我们使用RNAi喂养方法对unc-34无突变突变体背景中的合成致死力进行了筛选。据我们所知,这是首次报道的基于RNAi的遗传相互作用子筛选。筛选的结果是,我们鉴定了第二种秀丽隐杆线虫WASP家族蛋白wve-1,该蛋白与SCAR / WAVE蛋白最同源。 wve-1功能受损的动物在胃排泄中表现出缺陷,无法进行适当的形态发生,并且在神经元细胞迁移和轴突生长方面表现出缺陷。降低unc-34 / ena或wsp-1突变体背景中的wve-1水平也会导致胃泌素和形态发生缺陷的显着增强。因此,unc-34 / ena,wsp-1和wve-1在胚胎发生过程中起重叠作用,而unc-34 / ena和wsp-1在神经元细胞迁移中起重叠作用。这些观察结果表明,WASP和Ena / VASP蛋白可以在体内相互补偿,并首次证明了Ena / VASP蛋白在胃形成和形态发生中的作用。此外,我们的结果提供了WASP家族蛋白在后生神经元细胞迁移和胞质分裂中体内作用的第一个例子。

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