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Requirements for F-BAR Proteins TOCA-1 and TOCA-2 in Actin Dynamics and Membrane Trafficking during Caenorhabditis elegans Oocyte Growth and Embryonic Epidermal Morphogenesis

机译:F-BAR蛋白TOCA-1和TOCA-2在秀丽隐杆线虫卵母细胞生长和胚胎表皮形态发生过程中的肌动蛋白动力学和膜运输中的要求

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摘要

The TOCA family of F-BAR–containing proteins bind to and remodel lipid bilayers via their conserved F-BAR domains, and regulate actin dynamics via their N-Wasp binding SH3 domains. Thus, these proteins are predicted to play a pivotal role in coordinating membrane traffic with actin dynamics during cell migration and tissue morphogenesis. By combining genetic analysis in Caenorhabditis elegans with cellular biochemical experiments in mammalian cells, we showed that: i) loss of CeTOCA proteins reduced the efficiency of Clathrin-mediated endocytosis (CME) in oocytes. Genetic interference with CeTOCAs interacting proteins WSP-1 and WVE-1, and other components of the WVE-1 complex, produced a similar effect. Oocyte endocytosis defects correlated well with reduced egg production in these mutants. ii) CeTOCA proteins localize to cell–cell junctions and are required for proper embryonic morphogenesis, to position hypodermal cells and to organize junctional actin and the junction-associated protein AJM-1. iii) Double mutant analysis indicated that the toca genes act in the same pathway as the nematode homologue of N-WASP/WASP, wsp-1. Furthermore, mammalian TOCA-1 and C. elegans CeTOCAs physically associated with N-WASP and WSP-1 directly, or WAVE2 indirectly via ABI-1. Thus, we propose that TOCA proteins control tissues morphogenesis by coordinating Clathrin-dependent membrane trafficking with WAVE and N-WASP–dependent actin-dynamics.
机译:含F-BAR的TOCA家族蛋白通过其保守的F-BAR结构域与脂质双层结合并重塑脂质双层,并通过其N-Wasp结合SH3结构域调节肌动蛋白动力学。因此,预计这些蛋白质在细胞迁移和组织形态发生过程中在协调膜运输和肌动蛋白动力学中起关键作用。通过将秀丽隐杆线虫的遗传分析与哺乳动物细胞中的细胞生化实验相结合,我们表明:i)CeTOCA蛋白的丢失降低了卵母细胞中网格蛋白介导的内吞作用(CME)的效率。 CeTOCAs相互作用蛋白WSP-1和WVE-1,以及WVE-1复合体的其他成分的遗传干扰产生了相似的效果。卵母细胞内吞缺陷与这些突变体的产卵量减少有很好的相关性。 ii)CeTOCA蛋白位于细胞间连接处,是正确的胚胎形态发生,定位皮下细胞,组织连接肌动蛋白和与连接相关的蛋白AJM-1所必需的。 iii)双重突变体分析表明toca基因的作用途径与N-WASP / WASP wsp-1的线虫同源物相同。此外,哺乳动物TOCA-1和秀丽隐杆线虫直接与N-WASP和WSP-1物理关联,或通过ABI-1间接与WAVE2物理关联。因此,我们建议TOCA蛋白通过与WAVE和N-WASP依赖的肌动蛋白动力学协调网格蛋白依赖的膜运输来控制组织形态发生。

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