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首页> 外文期刊>International Journal of Quantum Chemistry >Molecular Dynamics Simulation on HP1 Protein Binding by Histone H3 Tail Methylation and Phosphorylation
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Molecular Dynamics Simulation on HP1 Protein Binding by Histone H3 Tail Methylation and Phosphorylation

机译:组蛋白H3尾甲基化和磷酸化对HP1蛋白结合的分子动力学模拟

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摘要

Trimethylation of histone H3 lysine 9 is important for recruiting heterochromatin protein 1 (HP1) to discrete regions of the genome, thereby regulating gene expression, chromatin packaging, and heterochromatin formation. Phosphorylation of histone H3 has been linked with mitotic chromatin condensation. During mitosis in vivo, H3 lysine 9 methylation and serine 10 phosphorylation can occur concomitantly on the same histone tail, whereas the influence of phosphorylation to trimethylation H3 tail recruiting HP1 remains controversial. In this work, molecular dynamics simulation of HP1 complexed with both trimethylated and phosphorylated H3 tail were performed and compared with the results from the previous methylated H3-HP1 trajectory. It is clear from the 10-ns dynamics simulation that two adjacent posttranslational modifications directly increase the flexibility of the H3 tail and weaken HP1 binding to chromatin. A combinatorial readout of two adjacent posttranslational modifications-a stable methylation and a dynamic phosphorylation mark-establish a regulatory mechanism of protein-protein interactions. (C) 2008 Wiley Periodicals, Inc. Int J Quantum Chem 109: 746-755, 2009
机译:组蛋白H3赖氨酸9的三甲基化对于将异染色质蛋白1(HP1)募集到基因组的离散区域很重要,从而调节基因表达,染色质包装和异染色质形成。组蛋白H3的磷酸化与有丝分裂染色质缩合有关。在体内有丝分裂期间,H3赖氨酸9甲基化和丝氨酸10磷酸化可同时发生在同一组蛋白尾巴上,而磷酸化对三甲基化H3尾巴募集HP1的影响仍然存在争议。在这项工作中,对与三甲基化和磷酸化的H3尾部复合的HP1进行了分子动力学模拟,并将其与先前甲基化的H3-HP1轨迹的结果进行了比较。从10 ns的动力学仿真中可以明显看出,两个相邻的翻译后修饰直接增加了H3尾部的柔韧性,并削弱了HP1与染色质的结合。两个相邻的翻译后修饰(稳定的甲基化和动态的磷酸化标记)的组合读数建立了蛋白质-蛋白质相互作用的调节机制。 (C)2008 Wiley Periodicals,Inc. Int J Quantum Chem 109:746-755,2009

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