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首页> 外文期刊>Genes to cells : >Essential requirement for RING finger E3 ubiquitin ligase Hakai in early embryonic development of Drosophila
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Essential requirement for RING finger E3 ubiquitin ligase Hakai in early embryonic development of Drosophila

机译:果蝇早期胚胎发育中RING手指E3泛素连接酶Hakai的基本要求

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摘要

Hakai is a RING finger type E3 ubiquitin ligase that is highly conserved in metazoans. Mammalian Hakai was shown to bind and ubiquitinate the intracellular domain of E-cadherin, and this activity is implicated in down-regulation of E-cadherin during v-Src-induced cellular transformation. To evaluate this model in vivo, we studied the function of the Drosophila homologue of Hakai. In cultured S2 cells, Drosophila Hakai and E-cadherin (Shotgun) formed a complex in a way distinct from the interaction described for mammalian counterparts. Hakai null mutants died during larval stages but this lethality could be offset by a HA-tagged Hakai construct. While zygotic Hakai function was dispensable for cell proliferation and differentiation in the wing disc epithelium, maternal Hakai mutants showed a variety of defects in epithelial integrity, including stochastic loss of E-cadherin expression and reduction of aPKC; defects in cell specification and cell migration were also observed. No increase of E-cadherin, however, was observed. Regulation of multiple target proteins under control of Hakai is, therefore, essential for early embryonic morphogenesis in Drosophila.
机译:Hakai是一种在后生动物中高度保守的RING手指E3型泛素连接酶。哺乳动物Hakai已显示出结合并泛素化E-钙粘蛋白的细胞内结构域,并且此活性与v-Src诱导的细胞转化过程中E-钙粘蛋白的下调有关。为了在体内评估该模型,我们研究了Hakai果蝇同源物的功能。在培养的S2细胞中,果蝇Hakai和E-钙粘蛋白(Shotgun)以不同于哺乳动物对应物的相互作用的方式形成复合物。 Hakai null突变体在幼虫阶段死亡,但是这种致命性可以被HA标签的Hakai构建体抵消。虽然合子的Hakai功能对于翼盘上皮细胞的增殖和分化是必不可少的,但母体的Hakai突变体在上皮完整性方面表现出多种缺陷,包括E-钙粘蛋白表达的随机丧失和aPKC的降低。还观察到细胞规格和细胞迁移方面的缺陷。然而,未观察到E-钙粘蛋白的增加。因此,在果蝇的控制下调节多种靶蛋白对于果蝇早期胚胎形态发生至关重要。

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