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MTA1在癌症进展和转移中的作用。

Role of MTA1 in cancer progression and metastasis.

作者信息

Sen Nirmalya, Gui Bin, Kumar Rakesh

机构信息

Department of Biochemistry and Molecular Medicine, George Washington University, Washington, DC, 20037, USA.

出版信息

Cancer Metastasis Rev. 2014 Dec;33(4):879-89. doi: 10.1007/s10555-014-9515-3.

Abstract

The MTA1 protein contributes to the process of cancer progression and metastasis through multiple genes and protein targets and interacting proteins with roles in transformation, anchorage-independent growth, invasion, survival, DNA repair, angiogenesis, hormone independence, metastasis, and therapeutic resistance. Because the roles and clinical significance of MTA proteins in human cancer are discussed by other contributors in this issue, this review will focus on our current understanding of the underlying principles of action behind the biological effects of MTA1. MTA proteins control a spectrum of cancer-promoting processes by modulating the expression of target genes and/or the activity of MTA-interacting proteins. In the case of MTA1, these functions are manifested through posttranslational modifications of MTA1 in response to upstream signals, MTA1 interaction with binding proteins, and the expression of target gene products. Studies delineating the molecular basis of dual functionality of MTA1 reveal that the functions of MTA1-chromatin-modifying complexes in the context of target gene regulation are dynamic in nature. The nature and targets of MTA1-chromatin-modifying complexes are also governed by the dynamic plasticity of the nucleosome landscape as well as kinetics of activation and inactivation of enzymes responsible for posttranslational modifications on the MTA1 protein. These broadly applicable functions also explain why MTA1 may be a "hub" gene in cancer. Because the deregulation of enzymes and their substrates with roles in MTA1 biology is not necessarily limited to cancer, we speculate that the lessons from MTA1 as a prototype dual master coregulator will be relevant for other human diseases. In this context, the concept of the dynamic nature of corepressor versus coactivator complexes and the MTA1 proteome as a function of time to signal is likely to be generally applicable to other multiprotein regulatory complexes in living systems.

摘要

MTA1蛋白通过多个基因、蛋白质靶点以及在转化、非锚定依赖性生长、侵袭、存活、DNA修复、血管生成、激素非依赖性、转移和治疗抗性中起作用的相互作用蛋白,参与癌症进展和转移过程。由于本期其他作者已讨论了MTA蛋白在人类癌症中的作用和临床意义,因此本综述将聚焦于我们目前对MTA1生物学效应背后作用基本原理的理解。MTA蛋白通过调节靶基因的表达和/或与MTA相互作用蛋白的活性,控制一系列促进癌症的过程。就MTA1而言,这些功能通过MTA1响应上游信号的翻译后修饰、MTA1与结合蛋白的相互作用以及靶基因产物的表达得以体现。描绘MTA1双重功能分子基础的研究表明,在靶基因调控背景下,MTA1染色质修饰复合物的功能本质上是动态的。MTA1染色质修饰复合物的性质和靶点还受核小体格局的动态可塑性以及负责MTA1蛋白翻译后修饰的酶的激活和失活动力学的支配。这些广泛适用的功能也解释了为什么MTA1可能是癌症中的一个“枢纽”基因。由于在MTA1生物学中起作用的酶及其底物的失调不一定仅限于癌症,我们推测,以MTA1作为双主核心调节因子原型所获得的经验教训将与其他人类疾病相关。在这种情况下,共抑制因子与共激活因子复合物以及MTA1蛋白质组随时间对信号响应的动态性质这一概念,可能普遍适用于生命系统中的其他多蛋白调节复合物。

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