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Rho GTPase信号通路在上皮折叠过程中被反复使用,并可能决定Rho激活的结果。

A Rho GTPase signaling pathway is used reiteratively in epithelial folding and potentially selects the outcome of Rho activation.

作者信息

Nikolaidou Kelly K, Barrett Kathy

机构信息

Ludwig Institute for Cancer Research, 91 Riding House Street, London W1W 7BS, United Kingdom.

出版信息

Curr Biol. 2004 Oct 26;14(20):1822-6. doi: 10.1016/j.cub.2004.09.080.

Abstract

A single Rho GTPase family member is capable of initiating several different processes, including cell cycle regulation, cytokinesis, cell migration, and transcriptional regulation . It is not clear, however, how the Rho protein selects which of these processes to initiate. Guanine nucleotide exchange factors (GEFs), proteins that activate Rho GTPases, could be important in making this selection. We show here that in vivo, DRhoGEF2, a GEF that is ubiquitously expressed and specific for Rho1, is reiteratively required for epithelial folding and invagination, but not for other processes regulated by Rho. The limitation of DRhoGEF2 function supports the hypothesis that the GEF selects the outcome of Rho activation. DRhoGEF2 exerts its effects in gastrulation through the regulation of Myosin II to orchestrate coordinated apical cell constriction. Apical myosin localization is also regulated by Concertina (Cta), a Galpha(12/13) family member that is thought to activate DRhoGEF2 and is itself activated by a putative ligand, Folded gastrulation (Fog). Fog and Cta also play a role in the morphogenetic events requiring DRhoGEF2, suggesting the existence of a conserved signaling pathway in which Fog, Cta, and DRhoGEF2 locally activate Myosin for epithelial invagination and folding.

摘要

单个Rho GTPase家族成员能够启动几种不同的过程,包括细胞周期调控、胞质分裂、细胞迁移和转录调控。然而,尚不清楚Rho蛋白如何选择启动这些过程中的哪一个。鸟嘌呤核苷酸交换因子(GEFs),即激活Rho GTPases的蛋白质,可能在做出这种选择中起重要作用。我们在此表明,在体内,DRhoGEF2,一种普遍表达且对Rho1具有特异性的GEF,对于上皮折叠和内陷是反复必需的,但对于由Rho调控的其他过程则不是必需的。DRhoGEF2功能的局限性支持了这样一种假设,即GEF选择Rho激活的结果。DRhoGEF2通过调节肌球蛋白II在原肠胚形成中发挥作用,以协调顶端细胞的收缩。顶端肌球蛋白的定位也受Concertina(Cta)调控,Cta是一种Gα(12/13)家族成员,被认为可激活DRhoGEF2,其本身又被一种假定的配体Folded gastrulation(Fog)激活。Fog和Cta在需要DRhoGEF2的形态发生事件中也发挥作用,这表明存在一条保守的信号通路,其中Fog、Cta和DRhoGEF2局部激活肌球蛋白以实现上皮内陷和折叠。

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