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The relationship between histone H3 phosphorylation and acetylation throughout the mammalian cell cycle

机译:整个哺乳动物细胞周期中组蛋白H3磷酸化与乙酰化之间的关系

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During interphase, histone amino-terminal tails play important roles in regulating the extent of DNA compaction. Post-translational modifications of the histone tails are intimately associated with regulating chromatin structure: phosphorylation of histone H3 is associated with proper chromosome condensation and dynamics during mitosis, while multiple H2B, H3, and H4 tail acetylations destabilize the chromatin fiber and are sufficient to decondense chromatin fibers in vitro. In this study, we investigate the spatio-temporal dynamics of specific histone H3 phosphorylations and acetylations to better understand the interplay of these post-translational modifications throughout the cell cycle. Using a panel of antibodies that individually, or in combination, recognize phosphorylated serines 10 and 28 and acetylated lysines 9 and 14, we define a series of changes associated with histone H3 that occur as cells progress through the cell cycle. Our results establish that mitosis appears to be a period of the cell cycle when many modifications are highly dynamic. Furthermore, they suggest that the upstream histone acetyltransferases/deacetylases and kinase/phosphatases are temporally regulated to alter their function globally during specific cell cycle time points.
机译:在相间期,组蛋白氨基末端的尾巴在调节DNA压缩程度方面起重要作用。组蛋白尾部的翻译后修饰与染色质结构的调节密切相关:组蛋白H3的磷酸化与有丝分裂过程中适当的染色体浓缩和动态相关,而多个H2B,H3和H4尾部乙酰化则使染色质纤维不稳定并足以解凝。染色质纤维体外。在这项研究中,我们调查了特定的组蛋白H3磷酸化和乙酰化的时空动态,以更好地了解整个细胞周期中这些翻译后修饰的相互作用。使用一组单独或组合识别磷酸化的丝氨酸10和28和乙酰化的赖氨酸9和14的抗体,我们定义了与组蛋白H3相关的一系列变化,这些变化随着细胞在整个细胞周期中的进展而发生。我们的结果表明,当许多修饰高度动态时,有丝分裂似乎是细胞周期的一个时期。此外,他们暗示上游组蛋白乙酰转移酶/脱乙酰酶和激酶/磷酸酶在特定的细胞周期时间点被暂时调节以整体改变其功能。

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