KDM4B mutations in human cancers

IF 1.5 4区医学 Q4 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Mutation Research-Fundamental and Molecular Mechanisms of Mutagenesis Pub Date : 2024-06-11 DOI:10.1016/j.mrfmmm.2024.111866

Wesley Bush , Korey Bosart , Renee A. Bouley , Ruben C. Petreaca

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Abstract

Homologous recombination (HR) is essential for repair of DNA double-strand breaks (DSBs) and restart of stalled or collapsed replication forks. Most cancers are characterized by mutations in components of the DSB repair pathways. Redundant DSB repair pathways exist in eukaryotes from yeast to humans and recent evidence has shown that complete loss of HR function appears to be lethal. Recent evidence has also shown that cancer cells with mutations in one DSB repair pathway can be killed by inhibiting one or more parallel pathways, a strategy that is currently aggressively explored as a cancer therapy. KDM4B is a histone demethylase with pleiotropic functions, which participates in preparing DSBs for repair by contributing to chromatin remodeling. In this report we carried out a pan-cancer analysis of KDM4B mutations with the goal of understanding their distribution and interaction with other DSB genes. We find that although KDM4B mutations co-occur with DSB repair genes, most KDM4B mutations are not drivers or pathogenic. A sequence conservation analysis from yeast to humans shows that highly conserved residues are resistant to mutation. Finally, all mutations occur in a heterozygous state. A single mutation, R986L, was predicted to significantly affect protein structure using computational modeling. This analysis suggests that KDM4B makes contributions to DSB repair but is not a key player.

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人类癌症中的 KDM4B 突变

同源重组（HR）对于 DNA 双链断裂（DSB）的修复以及停滞或崩溃的复制叉的重启至关重要。大多数癌症的特征是DSB修复途径中的成分发生了突变。从酵母到人类，真核生物中都存在冗余的 DSB 修复途径，最近的证据表明，完全丧失 HR 功能似乎是致命的。最近的证据还表明，一种 DSB 修复途径发生突变的癌细胞可以通过抑制一种或多种平行途径而被杀死，这种策略目前正被积极探索作为癌症疗法。KDM4B 是一种具有多种功能的组蛋白去甲基化酶，它通过参与染色质重塑，为 DSB 修复做好准备。在本报告中，我们对 KDM4B 突变进行了泛癌症分析，目的是了解它们的分布以及与其他 DSB 基因的相互作用。我们发现，虽然KDM4B突变与DSB修复基因共存，但大多数KDM4B突变不是驱动基因或致病基因。从酵母到人类的序列保守性分析表明，高度保守的残基对突变具有抵抗力。最后，所有突变都发生在杂合状态。通过计算建模，预测 R986L 这一单一突变会显著影响蛋白质结构。这项分析表明，KDM4B 对 DSB 修复有贡献，但不是关键角色。

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来源期刊

Mutation Research-Fundamental and Molecular Mechanisms of Mutagenesis 生物-毒理学

CiteScore

4.90

自引率

0.00%

发文量

审稿时长

51 days

期刊介绍： Mutation Research (MR) provides a platform for publishing all aspects of DNA mutations and epimutations, from basic evolutionary aspects to translational applications in genetic and epigenetic diagnostics and therapy. Mutations are defined as all possible alterations in DNA sequence and sequence organization, from point mutations to genome structural variation, chromosomal aberrations and aneuploidy. Epimutations are defined as alterations in the epigenome, i.e., changes in DNA methylation, histone modification and small regulatory RNAs. MR publishes articles in the following areas: Of special interest are basic mechanisms through which DNA damage and mutations impact development and differentiation, stem cell biology and cell fate in general, including various forms of cell death and cellular senescence. The study of genome instability in human molecular epidemiology and in relation to complex phenotypes, such as human disease, is considered a growing area of importance. Mechanisms of (epi)mutation induction, for example, during DNA repair, replication or recombination; novel methods of (epi)mutation detection, with a focus on ultra-high-throughput sequencing. Landscape of somatic mutations and epimutations in cancer and aging. Role of de novo mutations in human disease and aging; mutations in population genomics. Interactions between mutations and epimutations. The role of epimutations in chromatin structure and function. Mitochondrial DNA mutations and their consequences in terms of human disease and aging. Novel ways to generate mutations and epimutations in cell lines and animal models.