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RHO to the DOCK for GDP disembarking: Structural insights into the DOCK GTPase nucleotide exchange factors

机译:Rho到码头用于GDP下船:对码头GTP酶的结构见解核苷酸核苷酸交换因子

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摘要

The human dedicator of cytokinesis (DOCK) family consists of 11 structurally conserved proteins that serve as atypical RHO guanine nucleotide exchange factors (RHO GEFs). These regulatory proteins act as mediators in numerous cellular cascades that promote cytoskeletal remodeling, playing roles in various crucial processes such as differentiation, migration, polarization, and axon growth in neurons. At the molecular level, DOCK DHR2 domains facilitate nucleotide dissociation from small GTPases, a process that is otherwise too slow for rapid spatiotemporal control of cellular signaling. Here, we provide an overview of the biological and structural characteristics for the various DOCK proteins and describe how they differ from other RHO GEFs and between DOCK subfamilies. The expression of the family varies depending on cell or tissue type, and they are consequently implicated in a broad range of disease phenotypes, particularly in the brain. A growing body of available structural information reveals the mechanism by which the catalytic DHR2 domain elicits nucleotide dissociation and also indicates strategies for the discovery and design of high-affinity small-molecule inhibitors. Such compounds could serve as chemical probes to interrogate the cellular function and provide starting points for drug discovery of this important class of enzymes.
机译:Cytokinesis(码头)家族的人类专用物由11种结构保守的蛋白质组成,该蛋白质是非典型Rho鸟嘌呤核苷酸交换因子(Rho Gefs)。这些调节蛋白在许多细胞级联中起到介质,促进细胞骨骼改造,在神经元中的分化,迁移,极化和轴突生长等各种关键方法中发挥作用。在分子水平,码头DHR2结构域促进来自小GTP酶的核苷酸解离,这是否则对于快速的蜂窝信号传导的时尚控制的过程。在这里,我们概述了各种码头蛋白的生物学和结构特征,并描述了它们与其他Rho Gefs的不同之处以及码头亚属植物之间的不同。家族的表达根据细胞或组织类型而变化,因此它们具有广泛的疾病表型,特别是在大脑中。一种成长的可用结构信息揭示了催化DHR2结构域引发核苷酸解离的机制,并表明了高亲和力小分子抑制剂的发现和设计的策略。这些化合物可以用作化学探针,以询问细胞功能,并为这类重要酶的药物发现提供起点。

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