首页> 外文期刊>The Journal of biological chemistry >Structure of the Shroom-Rho Kinase Complex Reveals a Binding Interface with Monomeric Shroom That Regulates Cell Morphology and Stimulates Kinase Activity
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Structure of the Shroom-Rho Kinase Complex Reveals a Binding Interface with Monomeric Shroom That Regulates Cell Morphology and Stimulates Kinase Activity

机译:Shroom-Rho激酶复合物的结构揭示了具有调节细胞形态并刺激激酶活性的单体舒适的结合界面

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Shroom-mediated remodeling of the actomyosin cytoskeleton is a critical driver of cellular shape and tissue morphology that underlies the development of many tissues including the neural tube, eye, intestines, and vasculature. Shroom uses a conserved SD2 domain to direct the subcellular localization of Rho-associated kinase (Rock), which in turn drives changes in the cytoskeleton and cellular morphology through its ability to phosphorylate and activate non-muscle myosin II. Here, we present the structure of the human Shroom-Rock binding module, revealing an unexpected stoichiometry for Shroom in which two Shroom SD2 domains bind independent surfaces on Rock. Mutation of interfacial residues impaired Shroom-Rock binding in vitro and resulted in altered remodeling of the cytoskeleton and loss of Shroom-mediated changes in cellular morphology. Additionally, we provide the first direct evidence that Shroom can function as a Rock activator. These data provide molecular insight into the Shroom-Rock interface and demonstrate that Shroom directly participates in regulating cytoskeletal dynamics, adding to its known role in Rock localization.
机译:Shroom介导的Actomyosin细胞骨架的重塑是细胞形状和组织形态的关键驾驶员,使许多组织的发展潜在,包括神经管,眼睛,肠道和血管系统。 Shroom使用保守的SD2结构域引导RHO相关激酶(岩石)的亚细胞定位,这反过来通过其磷酸化和激活非肌肉肌蛋白II的能力来驱动细胞骨架和细胞形态的变化。在这里,我们介绍了人类的血管岩粘结模块的结构,揭示了Shroom的意外化学计量,其中两个Shroom SD2域在岩石上结合独立的表面。界面残留物的突变在体外损害血管岩结合受损,导致细胞骨架的改变改变的细胞骨架和血管内介导变化的丧失。此外,我们提供了第一个直接证据,即Shroom可以用作岩石激活物。这些数据为Shroom-Rock界面提供了分子洞察力,并证明Shroom直接参与调节细胞骨骼动态,并在岩石定位中增加了其已知作用。

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