大脑功能中与衰老相关的组蛋白修饰变化。

Ibrain Pub Date : 2023-05-17 DOI:10.1002/ibra.12106
Yanwen Ding, Chengxi Liu, Yi Zhang
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引用次数: 0

摘要

衰老可以定义为更难逆转的生理功能下降,其特征是随着时间的推移,生物体的组织、器官和细胞的生理完整性丧失。正常衰老与大脑的结构和功能变化有关,包括神经元凋亡、突触结构、神经传递和代谢改变,导致睡眠、认知功能、记忆、学习、运动和感觉系统受损。组蛋白修饰是一种与衰老相关的显著表观遗传学变化,影响大脑的突触和线粒体功能以及免疫和应激反应。这篇综述讨论了大脑衰老过程中发生的组蛋白修饰的变化,特别是甲基化和乙酰化,以及基因转录和蛋白质表达的相关变化。我们观察到,在衰老的大脑中,与突触和线粒体功能相关的基因下调,而与免疫反应和炎症功能有关的基因上调。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Aging-related histone modification changes in brain function

Aging can be defined as a decline of physiological function that is more difficult to reverse, characterized by the loss of the physiological integrity of tissues, organs, and cells of an organism over time. Normal aging is associated with structural and functional changes in the brain, involving neuronal apoptosis, synaptic structure, neurotransmission, and metabolism alterations, leading to impairment in sleep, cognitive functions, memory, learning, and motor and sensory systems. Histone modification is a significant aging-related epigenetic change that influences synaptic and mitochondrial function and immune and stress responses in the brain. This review discusses the changes in histone modifications that occur during brain aging, specifically methylation and acetylation, and the associated changes in gene transcription and protein expression. We observed that genes related to synaptic and mitochondrial function are downregulated in the aging brain, while genes related to immune response and inflammatory functions are upregulated.

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