组蛋白
染色质
核小体
生物
乙酰化
组蛋白密码
细胞生物学
组蛋白H1
组蛋白H4
组蛋白八聚体
芽殖酵母
组蛋白甲基化
组蛋白H2A
组蛋白甲基转移酶
遗传学
酵母
酿酒酵母
DNA
基因表达
基因
DNA甲基化
作者
Mithun Mitra,Hilary A. Coller
出处
期刊:FEBS Journal
[Wiley]
日期:2023-05-15
卷期号:290 (14): 3533-3538
摘要
Quiescence, reversible cell cycle arrest, is essential for survival during nutrient limitations and the execution of precise developmental patterns. In yeast, entry into quiescence is associated with a loss of histone acetylation as the chromatin becomes tightly condensed. In this issue, Small and Osley performed an unbiased screen of mutations in histone H3 and H4 amino acids in budding yeast and identified histone residues that are critical for quiescence and chronological lifespan. The results indicate that multiple histone amino acids, likely affecting nucleosome structure and a wide range of chromatin-associated processes, can promote or inhibit quiescence entry. Many of the same histone amino acids are also critical regulators of chronological lifespan.
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