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引用次数: 0
摘要
组蛋白对维持染色质结构和功能至关重要。组蛋白突变会导致染色质压实、基因表达和 DNA 修复蛋白被招募到 DNA 病变部位。这些破坏会损害关键的 DNA 修复途径,如同源重组和非同源末端连接,导致基因组不稳定性增加,从而形成有利于肿瘤发生和发展的环境。了解了这些机制后,我们就可以针对携带突变组蛋白的癌症中的DNA修复途径,提供新的治疗策略,利用其固有的基因组不稳定性获得更好的治疗效果。在这里,我们将研究组蛋白H3的突变如何破坏正常的染色质功能和DNA损伤修复过程,以及如何利用这些机制进行治疗干预。
Histone H3 mutations and their impact on genome stability maintenance.
Histones are essential for maintaining chromatin structure and function. Histone mutations lead to changes in chromatin compaction, gene expression, and the recruitment of DNA repair proteins to the DNA lesion. These disruptions can impair critical DNA repair pathways, such as homologous recombination and non-homologous end joining, resulting in increased genomic instability, which promotes an environment favorable to tumor development and progression. Understanding these mechanisms underscores the potential of targeting DNA repair pathways in cancers harboring mutated histones, offering novel therapeutic strategies to exploit their inherent genomic instability for better treatment outcomes. Here, we examine how mutations in histone H3 disrupt normal chromatin function and DNA damage repair processes and how these mechanisms can be exploited for therapeutic interventions.
期刊介绍:
Biochemical Society Transactions is the reviews journal of the Biochemical Society. Publishing concise reviews written by experts in the field, providing a timely snapshot of the latest developments across all areas of the molecular and cellular biosciences.
Elevating our authors’ ideas and expertise, each review includes a perspectives section where authors offer comment on the latest advances, a glimpse of future challenges and highlighting the importance of associated research areas in far broader contexts.