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转录抑制及其他过程中反复出现的磷酸化-类泛素化开关

A recurrent phospho-sumoyl switch in transcriptional repression and beyond.

作者信息

Yang Xiang-Jiao, Grégoire Serge

机构信息

Molecular Oncology Group, Department of Medicine, McGill University Health Center, Montréal, Quebec H3A 1A1, Canada.

出版信息

Mol Cell. 2006 Sep 15;23(6):779-86. doi: 10.1016/j.molcel.2006.08.009.

Abstract

How multisite posttranslational modification coordinates dynamic regulation of protein function is an issue fundamental to many biological processes. Related to this, a composite sequence motif has recently been identified that couples phosphorylation, sumoylation, and perhaps also deacetylation to control transcriptional repression in stress response, mitogen and nuclear hormone signaling, myogenesis, and neuronal differentiation. This motif is present in many proteins, integrates cellular signals from diverse pathways, and serves as a valuable signature for in silico identification of proteins regulated by adjacent phosphorylation and sumoylation.

摘要

多位点翻译后修饰如何协调蛋白质功能的动态调节是许多生物学过程的一个基本问题。与此相关的是,最近发现了一种复合序列基序,它将磷酸化、SUMO化以及可能的去乙酰化耦合起来,以控制应激反应、有丝分裂原和核激素信号传导、肌生成和神经元分化中的转录抑制。这个基序存在于许多蛋白质中,整合来自不同途径的细胞信号,并作为一个有价值的标记,用于在计算机上识别受相邻磷酸化和SUMO化调节的蛋白质。

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