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Rho GTP 酶鸟嘌呤核苷酸交换因子(RhoGEFs)作为致癌效应物以及转移性癌症的战略治疗靶点。

Guanine nucleotide exchange factors for Rho GTPases (RhoGEFs) as oncogenic effectors and strategic therapeutic targets in metastatic cancer.

机构信息

Department of Pharmacology, CINVESTAV-IPN, Mexico City, Mexico.

Department of Pharmacology, CINVESTAV-IPN, Mexico City, Mexico.

出版信息

Cell Signal. 2023 Sep;109:110749. doi: 10.1016/j.cellsig.2023.110749. Epub 2023 Jun 7.

DOI:10.1016/j.cellsig.2023.110749
PMID:37290677
Abstract

Metastatic cancer cells dynamically adjust their shape to adhere, invade, migrate, and expand to generate secondary tumors. Inherent to these processes is the constant assembly and disassembly of cytoskeletal supramolecular structures. The subcellular places where cytoskeletal polymers are built and reorganized are defined by the activation of Rho GTPases. These molecular switches directly respond to signaling cascades integrated by Rho guanine nucleotide exchange factors (RhoGEFs), which are sophisticated multidomain proteins that control morphological behavior of cancer and stromal cells in response to cell-cell interactions, tumor-secreted factors and actions of oncogenic proteins within the tumor microenvironment. Stromal cells, including fibroblasts, immune and endothelial cells, and even projections of neuronal cells, adjust their shapes and move into growing tumoral masses, building tumor-induced structures that eventually serve as metastatic routes. Here we review the role of RhoGEFs in metastatic cancer. They are highly diverse proteins with common catalytic modules that select among a variety of homologous Rho GTPases enabling them to load GTP, acquiring an active conformation that stimulates effectors controlling actin cytoskeleton remodeling. Therefore, due to their strategic position in oncogenic signaling cascades, and their structural diversity flanking common catalytic modules, RhoGEFs possess unique characteristics that make them conceptual targets of antimetastatic precision therapies. Preclinical proof of concept, demonstrating the antimetastatic effect of inhibiting either expression or activity of βPix (ARHGEF7), P-Rex1, Vav1, ARHGEF17, and Dock1, among others, is emerging.

摘要

转移性癌细胞会动态调整其形状以黏附、侵袭、迁移和扩张,从而形成继发性肿瘤。在这些过程中,细胞骨架的超分子结构不断地组装和拆卸。细胞骨架聚合物构建和重新组织的亚细胞位置由 Rho GTPases 的激活所定义。这些分子开关直接响应由 Rho 鸟嘌呤核苷酸交换因子(RhoGEFs)整合的信号级联反应,RhoGEFs 是复杂的多结构域蛋白,可控制癌症和基质细胞的形态行为,以响应细胞-细胞相互作用、肿瘤分泌的因子以及肿瘤微环境中致癌蛋白的作用。基质细胞,包括成纤维细胞、免疫细胞和内皮细胞,甚至神经元细胞的突起,都会调整它们的形状并进入生长中的肿瘤块,构建肿瘤诱导的结构,最终作为转移途径。在这里,我们回顾了 RhoGEFs 在转移性癌症中的作用。它们是高度多样化的蛋白质,具有共同的催化模块,可以在各种同源 Rho GTPases 之间进行选择,使它们能够加载 GTP,获得刺激控制肌动蛋白细胞骨架重塑的效应物的活性构象。因此,由于它们在致癌信号级联反应中的战略位置,以及它们围绕共同催化模块的结构多样性,RhoGEFs 具有独特的特征,使它们成为抗转移精准治疗的概念性靶点。抑制βPix(ARHGEF7)、P-Rex1、Vav1、ARHGEF17 和 Dock1 等表达或活性的临床前概念验证,正在出现。

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