组蛋白:劫持组蛋白代码。

IF 4.7 2区 医学 Q1 ONCOLOGY
Varun Sahu, Chao Lu
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引用次数: 5

摘要

染色质功能障碍与越来越多的癌症有关,特别是在儿童和年轻人中。除了染色质修饰和重塑酶,组蛋白基因的突变也与人类癌症有关。自首次报道影响组蛋白H3尾部关键残基的热点错义突变以来,研究揭示了这些所谓的“癌组蛋白”是如何显性地(H3K27M和H3K36M)或局部地(H3.3G34R/W)抑制相应的组蛋白甲基转移酶并错调控表观基因组和转录组,从而促进肿瘤发生的。最近,在不同的癌症类型中发现了所有四种核心组蛋白的广泛突变。此外,一种“癌组蛋白样”蛋白EZHIP通过一种高度类似于H3K27M突变的机制参与了儿童室管膜瘤的发生。我们将回顾最近在了解典型和新型组蛋白突变的生化、分子和生物学机制方面的进展。重要的是,这些机制的见解已经确定了肿瘤组蛋白驱动肿瘤的治疗机会。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Oncohistones: Hijacking the histone code.

Oncohistones: Hijacking the histone code.

Oncohistones: Hijacking the histone code.

Chromatin dysfunction has been implicated in a growing number of cancers especially in children and young adults. In addition to chromatin modifying and remodeling enzymes, mutations in histone genes are linked to human cancers. Since the first reports of hotspot missense mutations affecting key residues at histone H3 tail, studies have revealed how these so-called "oncohistones" dominantly (H3K27M and H3K36M) or locally (H3.3G34R/W) inhibit corresponding histone methyltransferases and misregulate epigenome and transcriptome to promote tumorigenesis. More recently, widespread mutations in all four core histones are identified in diverse cancer types. Furthermore, an "oncohistone-like" protein EZHIP has been implicated in driving childhood ependymomas through a mechanism highly reminiscent of H3K27M mutation. We will review recent progresses on understanding the biochemical, molecular and biological mechanisms underlying the canonical and novel histone mutations. Importantly, these mechanistic insights have identified therapeutic opportunities for oncohistone-driven tumors.

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来源期刊
CiteScore
14.50
自引率
1.30%
发文量
13
期刊介绍: The Annual Review of Cancer Biology offers comprehensive reviews on various topics within cancer research, covering pivotal and emerging areas in the field. As our understanding of cancer's fundamental mechanisms deepens and more findings transition into targeted clinical treatments, the journal is structured around three main themes: Cancer Cell Biology, Tumorigenesis and Cancer Progression, and Translational Cancer Science. The current volume of this journal has transitioned from gated to open access through Annual Reviews' Subscribe to Open program, ensuring all articles are published under a CC BY license.
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