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p53:共价修饰在癌症中的多方面作用

p53: The Multifaceted Roles of Covalent Modifications in Cancer.

作者信息

Grigoreva Tatiana A, Romanova Angelina A, Tribulovich Vyacheslav G, Pestov Nikolay B, Oganov Ruslan A, Kovaleva Diana K, Korneenko Tatyana V, Barlev Nickolai A

机构信息

St. Petersburg State Institute of Technology, St-Petersburg 190013, Russia.

Institute of Biomedical Chemistry, Moscow 119121, Russia.

出版信息

Pharmaceuticals (Basel). 2024 Dec 13;17(12):1682. doi: 10.3390/ph17121682.

Abstract

The p53 protein has attracted huge research interest over several decades due to its role as one of the most important tumor suppressors in mammals, which orchestrates a synchronous response from normal cells in the body to various forms of stress. The diverse cellular activities of the p53 protein are regulated mainly via its post-translational modifications (PTMs). PTMs affect p53 on several levels: at the level of the assembly of tetrameric complexes on DNA to transactivate its target genes, at the level of the assembly of tetrameric complexes on DNA to transactivate its target genes; at the level of proteolysis in the absence of stress; and on the contrary, at the level of augmented protein stability in response to stress signals. Disruptions in these regulatory mechanisms can lead to deviations from normal cellular function, boosting tumor initiation and progression. Conversely, targeted interventions in these pathways could prove beneficial for the development of antitumor therapies. Advancing our understanding of p53 modifiers and the proteins involved in its regulation equips researchers with an expanded toolkit for studying cellular processes and for developing biologically active molecules that influence p53-mediated responses.

摘要

几十年来,p53蛋白一直吸引着大量的研究兴趣,因为它是哺乳动物中最重要的肿瘤抑制因子之一,能协调体内正常细胞对各种形式应激的同步反应。p53蛋白多样的细胞活性主要通过其翻译后修饰(PTM)来调节。PTM在多个层面影响p53:在DNA上组装四聚体复合物以激活其靶基因的层面;在无应激时的蛋白水解层面;相反,在响应应激信号时增强蛋白稳定性的层面。这些调节机制的破坏会导致细胞正常功能出现偏差,促进肿瘤的起始和进展。相反,对这些途径进行靶向干预可能对抗肿瘤治疗的发展有益。加深我们对p53修饰因子及其调控相关蛋白的理解,为研究人员提供了一个更丰富的工具集,用于研究细胞过程以及开发影响p53介导反应的生物活性分子。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bfcc/11677429/c56341d33871/pharmaceuticals-17-01682-g001.jpg

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