突变型 TRP53 发挥靶基因选择性显性负效应，驱动肿瘤发生。

Mutant TRP53 exerts a target gene-selective dominant-negative effect to drive tumor development.

机构信息

Walter and Eliza Hall Institute of Medical Research, Parkville, Melbourne, Victoria 3052, Australia.

Department of Medical Biology, University of Melbourne, Parkville, Melbourne, Victoria 3050, Australia.

出版信息

Genes Dev. 2018 Nov 1;32(21-22):1420-1429. doi: 10.1101/gad.314286.118. Epub 2018 Oct 26.

DOI:10.1101/gad.314286.118

PMID:30366906

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6217734/

Abstract

Mutations in , prevalent in human cancer, are reported to drive tumorigenesis through dominant-negative effects (DNEs) over wild-type TRP53 function as well as neomorphic gain-of-function (GOF) activity. We show that five TRP53 mutants do not accelerate lymphomagenesis on a TRP53-deficient background but strongly synergize with c-MYC overexpression in a manner that distinguishes the hot spot mutations. RNA sequencing revealed that the mutant TRP53 DNE does not globally repress wild-type TRP53 function but disproportionately impacts a subset of wild-type TRP53 target genes. Accordingly, TRP53 mutant proteins impair pathways for DNA repair, proliferation, and metabolism in premalignant cells. This reveals that, in our studies of lymphomagenesis, mutant TRP53 drives tumorigenesis primarily through the DNE, which modulates wild-type TRP53 function in a manner advantageous for neoplastic transformation.

摘要

在人类癌症中普遍存在的突变被报道通过对野生型 TRP53 功能的显性负效应 (DNE) 以及新功能获得 (GOF) 活性来驱动肿瘤发生。我们表明，五种 TRP53 突变体在 TRP53 缺陷背景下不会加速淋巴瘤的发生，但在 c-MYC 过表达的情况下会强烈协同作用，这种方式可以区分热点突变。RNA 测序表明，突变型 TRP53 的 DNE 不会全局抑制野生型 TRP53 功能，而是不成比例地影响野生型 TRP53 靶基因的一部分。因此，TRP53 突变蛋白会损害恶性前体细胞中的 DNA 修复、增殖和代谢途径。这表明，在我们对淋巴瘤发生的研究中，突变型 TRP53 主要通过 DNE 驱动肿瘤发生，这种方式以有利于肿瘤转化的方式调节野生型 TRP53 功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6bb6/6217734/e0f4c97021cd/1420f01.jpg

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突变型 TRP53 发挥靶基因选择性显性负效应，驱动肿瘤发生。

Mutant TRP53 exerts a target gene-selective dominant-negative effect to drive tumor development.

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