Global changes in and characterization of specific sites of phosphorylation in mouse and human histone H1 Isoforms upon CDK inhibitor treatment using mass spectrometry

使用质谱法分析小鼠和人类组蛋白 H1 异构体在 CDK 抑制剂处理后发生的整体变化及其磷酸化特定位点的表征

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作者:Leesa J Deterding, Maureen K Bunger, Geoffrey C Banks, Kenneth B Tomer, Trevor K Archer

Abstract

Global changes in the phosphorylation state of human H1 isoforms isolated from UL3 cells have been investigated using mass spectrometry. Relative changes in H1 phosphorylation between untreated cells and cells treated with dexamethasone or various CDK inhibitors were determined. The specific cyclin-dependent kinase consensus sites of phosphorylation on the histone H1 isoforms that show changes in phosphorylation were also investigated. Three sites of phosphorylation on histone H1.4 isoforms have been identified.

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