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The histone variant H3.3 claims its place in the crowded scene of epigenetics

机译:组蛋白变体H3.3在表观遗传学的拥挤场景中占据一席之地

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摘要

Histones are evolutionarily conserved DNA-binding proteins. As scaffolding molecules, they significantly regulate the DNA packaging into the nucleus of all eukaryotic cells. As docking units, they influence the recruitment of the transcriptional machinery, thus establishing unique gene expression patterns that ultimately promote different biological outcomes. While canonical histones H3.1 and H3.2 are synthetized and loaded during DNA replication, the histone variant H3.3 is expressed and deposited into the chromatin throughout the cell cycle. Recent findings indicate that H3.3 replaces the majority of canonical H3 in non-dividing cells, reaching almost saturation levels in a time-dependent manner. Consequently, H3.3 incorporation and turnover represent an additional layer in the regulation of the chromatin landscape during aging. In this respect, work from our group and others suggest that H3.3 plays an important function in age-related processes throughout evolution. Here, we summarize the current knowledge on H3.3 biology and discuss the implications of its aberrant dynamics in the establishment of cellular states that may lead to human pathology. Critically, we review the importance of H3.3 turnover as part of epigenetic events that influence senescence and age-related processes. We conclude with the emerging evidence that H3.3 is required for proper neuronal function and brain plasticity.
机译:组蛋白是进化上保守的DNA结合蛋白。作为支架分子,它们显着调节DNA包装入所有真核细胞核中的能力。作为对接单元,它们影响转录机制的募集,从而建立最终促进不同生物学结果的独特基因表达模式。在DNA复制过程中合成并加载了典型的组蛋白H3.1和H3.2,而组蛋白变体H3.3在整个细胞周期中均表达并沉积在染色质中。最近的发现表明,H3.3取代了非分裂细胞中的大多数规范H3,并以时间依赖的方式达到了几乎饱和的水平。因此,H3.3的掺入和周转代表了衰老过程中染色质景观调控的另一层。在这方面,我们小组和其他人的研究表明,H3.3在整个进化过程中与年龄相关的过程中起着重要作用。在这里,我们总结了有关H3.3生物学的最新知识,并讨论了其异常动力学在可能导致人类病理的细胞状态建立中的意义。至关重要的是,我们回顾了H3.3转换作为影响衰老和与年龄相关的过程的表观遗传事件的一部分的重要性。我们以新出现的证据得出结论,H3.3是正常神经元功能和大脑可塑性所必需的。

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