Litcius/Paper detail

Oncohistones: Hijacking the Histone Code

Varun Sahu, Chao Lü

2022Annual Review of Cancer Biology41 citationsDOIOpen Access PDF

Abstract

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.

Topics & Concepts

EpigenomeHistoneBiologyChromatinEpigeneticsGeneticsHistone codeCarcinogenesisHistone methyltransferaseEpigenomicsTranscriptomeChromatin remodelingHistone H3Computational biologyGeneCancer researchDNA methylationGene expressionNucleosomeGenomics and Chromatin DynamicsProtein Degradation and InhibitorsHistone Deacetylase Inhibitors Research