Regulation of Ras-GTPase Signaling and Localization by Post-Translational Modifications

A. Nair, Bhaskar Saha
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引用次数: 1

Abstract

Ras, a GTP-GDP binary switch protein, transduces signals from diverse receptors to regulate various signaling networks. Three Ras genes encode for protein isoforms, namely, Harvey Ras (H-Ras), Kirsten Ras (K-Ras, with two splice variants, K-Ras4A and K-Ras4B), and Neuroblastoma Ras (N-Ras). The isoforms undergo a series of post-translational modifications that enable their membrane attachment and biological activity. The activation of Ras isoforms is tightly regulated, and any dysregulation affects cellular processes, such as cell division, apoptosis, differentiation, cell migration, etc. The Ras gene is highly prone to mutation, and ~30% of cancers carry somatic mutations in Ras, whereas germline mutations clinically manifest as various rasopathies. In addition to regulation by the Guanine nucleotide exchange factors and the GTPase activation proteins, Ras signaling, and localization are also regulated by phosphorylation-dephosphorylation, ubiquitination, nitrosylation, and acetylation. Herein, we review the regulation of Ras signaling and localization by various regulatory enzymes in depth and assess the current status of Ras drug discovery targeting these regulatory enzymes.
翻译后修饰对Ras-GTPase信号转导和定位的调控
Ras是一种GTP-GDP二进制开关蛋白,它可以转导来自不同受体的信号来调节各种信号网络。三个Ras基因编码蛋白同工型,即Harvey Ras (H-Ras)、Kirsten Ras (K-Ras,有两个剪接变体,K-Ras4A和K-Ras4B)和神经母细胞瘤Ras (N-Ras)。同种异构体经过一系列的翻译后修饰,使其能够附着在膜上并具有生物活性。Ras亚型的激活受到严格调控,任何失调都会影响细胞过程,如细胞分裂、凋亡、分化、细胞迁移等。Ras基因极易突变,约30%的癌症携带Ras体细胞突变,而种系突变在临床上表现为各种rasopathies。除了受鸟嘌呤核苷酸交换因子和GTPase激活蛋白的调控外,Ras信号传导和定位还受磷酸化-去磷酸化、泛素化、亚硝基化和乙酰化的调控。本文就多种调控酶对Ras信号的调控及定位进行了综述,并对目前针对这些调控酶的Ras药物开发现状进行了评估。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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