Semenov Oleg, Daks Alexandra, Fedorova Olga, Shuvalov Oleg, Barlev Nickolai A
Regulation of Gene Expression Laboratory, Institute of Cytology RAS, Saint-Petersburg, Russia.
Laboratory of Intracellular Signalling, Moscow Institute of Physics and Technology, Dolgoprudny, Russia.
Front Mol Biosci. 2022 Jun 23;9:928399. doi: 10.3389/fmolb.2022.928399. eCollection 2022.
The central role of an aberrantly activated EMT program in defining the critical features of aggressive carcinomas is well documented and includes cell plasticity, metastatic dissemination, drug resistance, and cancer stem cell-like phenotypes. The p53 tumor suppressor is critical for leashing off all the features mentioned above. On the molecular level, the suppression of these effects is exerted by p53 via regulation of its target genes, whose products are involved in cell cycle, apoptosis, autophagy, DNA repair, and interactions with immune cells. Importantly, a set of specific mutations in the TP53 gene (named Gain-of-Function mutations) converts this tumor suppressor into an oncogene. In this review, we attempted to contrast different regulatory roles of wild-type and mutant p53 in the multi-faceted process of EMT.
异常激活的上皮-间质转化(EMT)程序在定义侵袭性癌的关键特征中所起的核心作用已得到充分证明,这些特征包括细胞可塑性、转移播散、耐药性以及癌症干细胞样表型。p53肿瘤抑制因子对于抑制上述所有特征至关重要。在分子水平上,p53通过调控其靶基因来发挥对这些效应的抑制作用,这些靶基因的产物参与细胞周期、凋亡、自噬、DNA修复以及与免疫细胞的相互作用。重要的是,TP53基因中的一组特定突变(称为功能获得性突变)将这种肿瘤抑制因子转化为一种癌基因。在本综述中,我们试图对比野生型和突变型p53在EMT多方面过程中的不同调控作用。
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