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Structural and Mechanistic Insights into the Regulation of the Fundamental Rho Regulator RhoGDIα by Lysine Acetylation

机译:赖氨酸乙酰化对基本Rho调节剂RhoGDIα调控的结构和机理研究

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摘要

Rho proteins are small GTP/GDP-binding proteins primarily involved in cytoskeleton regulation. Their GTP/GDP cycle is often tightly connected to a membrane/cytosol cycle regulated by the Rho guanine nucleotide dissociation inhibitor α (RhoGDIα). RhoGDIα has been regarded as a housekeeping regulator essential to control homeostasis of Rho proteins. Recent proteomic screens showed that RhoGDIα is extensively lysine-acetylated. Here, we present the first comprehensive structural and mechanistic study to show how RhoGDIα function is regulated by lysine acetylation. We discover that lysine acetylation impairs Rho protein binding and increases guanine nucleotide exchange factor-catalyzed nucleotide exchange on RhoA, these two functions being prerequisites to constitute a bona fide GDI displacement factor. RhoGDIα acetylation interferes with Rho signaling, resulting in alteration of cellular filamentous actin. Finally, we discover that RhoGDIα is endogenously acetylated in mammalian cells, and we identify CBP, p300, and pCAF as RhoGDIα-acetyltransferases and Sirt2 and HDAC6 as specific deacetylases, showing the biological significance of this post-translational modification.
机译:Rho蛋白是主要参与细胞骨架调节的小GTP / GDP结合蛋白。它们的GTP / GDP周期通常与受Rho鸟嘌呤核苷酸解离抑制剂α(RhoGDIα)调节的膜/细胞溶胶周期紧密相关。 RhoGDIα被认为是控制Rho蛋白体内平衡必不可少的管家调节剂。最近的蛋白质组学筛选显示RhoGDIα被赖氨酸广泛乙酰化。在这里,我们提出了第一个全面的结构和机理研究,以显示赖氨酸乙酰化如何调节RhoGDIα功能。我们发现,赖氨酸乙酰化会损害Rho蛋白结合,并增加RhoA上鸟嘌呤核苷酸交换因子催化的核苷酸交换,这两个功能是构成真正GDI置换因子的前提。 RhoGDIα乙酰化会干扰Rho信号传导,导致细胞丝状肌动蛋白发生改变。最后,我们发现RhoGDIα在哺乳动物细胞中被内源性乙酰化,并且我们将CBP,p300和pCAF识别为RhoGDIα-乙酰基转移酶,并将Sirt2和HDAC6识别为特定的脱乙酰基酶,显示了这种翻译后修饰的生物学意义。

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