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RhoA acts downstream of Wnt5 and Wnt1 to regulate convergence and extension movements by involving effectors Rho Kinase and Diaphanous: Use of zebrafish as an in vivo model for GTPase signaling

机译:RhoA在Wnt5和Wnt1下游起作用,通过参与效应子Rho Kinase和Diaphanous来调节会聚和延伸运动:使用斑马鱼作为GTPase信号转导的体内模型

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Gastrulation shapes the early embryos by forming three germ layers, ectoderm, mesoderm and endoderm. In vertebrates, this process requires massive cell rearrangement including convergence and extension (CE) movements that involve narrowing and lengthening of embryonic tissues as well as cell elongation. Such polarization and movements require precise reorganization and regulation of the cytoskeleton network and cell adhesion. Rho small GTPases are key regulators for dynamic actin cytoskeleton. However, the signaling mechanisms underlying their functions in CE remain to be further elucidated. We have cloned the zebrafish Danio rerio rhoA and by capitalizing on the specific functional knockdown using morpholmos against rhoA and the availability of CE mutants defective in Writ signaling, we showed that rhoA morphants were reminiscent to noncanonical wnt mutants with serious disruption in CE movements. Injection of rhoA mRNA effectively rescued such defects in wnt5 and wnt11 mutants. Furthermore, CE defects in rhoA knockdown or wnt mutants can be suppressed through functional bypass after ectopic expression of the two mammalian Rho effectors, the Rho kinase and Diaphanous (mDia). These results provide the first evidence that the RhoA in vivo acts downstream of Wnt5 and Wnt11 to effect, without affecting cell fates, on the CE movements in zebrafish embryos. Significantly, it elicits such effect via both effectors, Rho kinase and Dia. These findings also support the versatility of the zebrafish as a model to further investigate the roles of various classes of small GTPases in regulating cell dynamics in vivo. (c) 2005 Elsevier Inc. All rights reserved.
机译:胚乳通过形成三个胚层,即外胚层,中胚层和内胚层来塑造早期胚胎。在脊椎动物中,此过程需要进行大规模的细胞重排,包括会聚和延伸(CE)运动,这涉及使胚胎组织变窄和变长以及细胞伸长。这种极化和运动需要细胞骨架网络和细胞粘附的精确重组和调节。 Rho小型GTPases是动态肌动蛋白细胞骨架的关键调节剂。但是,它们在CE中的功能所基于的信令机制还有待进一步阐明。我们已经克隆了斑马鱼Danio rerio rhoA,并利用吗啡对rhoA的特异功能敲除以及Writ信号缺陷的CE突变体的可用性,证明了rhoA morphant令人联想到非典型的wnt突变体,其CE运动受到严重破坏。注射rhoA mRNA可有效挽救wnt5和wnt11突变体中的此类缺陷。此外,在两个哺乳动物Rho效应子Rho激酶和Diaphanous(mDia)异位表达后,可以通过功能旁路抑制rhoA组合或wnt突变体中的CE缺陷。这些结果提供了第一个证据,证明RhoA在体内作用于Wnt5和Wnt11的下游,而不影响细胞的命运,对斑马鱼胚胎中的CE运动产生影响。显着地,它通过Rho激酶和Dia这两种效应子引起这种效应。这些发现也支持斑马鱼作为模型的多功能性,以进一步研究各类小GTPases在调节体内细胞动力学中的作用。 (c)2005 Elsevier Inc.保留所有权利。

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