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四种不同的细胞周期蛋白依赖性激酶在组蛋白H1所有与生长相关的磷酸化位点使其磷酸化。

Four distinct cyclin-dependent kinases phosphorylate histone H1 at all of its growth-related phosphorylation sites.

作者信息

Swank R A, Th'ng J P, Guo X W, Valdez J, Bradbury E M, Gurley L R

机构信息

School of Medicine, Department of Biological Chemistry, University of California-Davis 95616, USA.

出版信息

Biochemistry. 1997 Nov 11;36(45):13761-8. doi: 10.1021/bi9714363.

Abstract

In mammalian cells, up to six serines and threonines in histone H1 are phosphorylated in vivo in a cell cycle dependent manner that has long been linked with chromatin condensation. Growth-associated H1 kinases, now known as cyclin-dependent kinases (CDKs), are thought to be the enzymes responsible for this process. This paper describes the phosphorylation of histone H1 by four different purified CDKs. The four CDKs phosphorylate only the cell cycle specific phosphorylation sites of H1, indicating that they belong to the kinase class responsible for growth-related H1 phosphorylation in vivo. All four CDKs phosphorylate all of the interphase and mitotic-specific H1 sites. In addition to the (S/T)PXK consensus phosphorylation sites, these four CDKs also phosphorylate a mitotic-specific in vivo H1 phosphorylation site that lacks this sequence. There is no site selectivity among the growth-related phosphorylation sites by any of the four CDKs because all four CDKs phosphorylate all relevant sites. The results imply that the cell cycle dependent H1 phosphorylations observed in vivo must involve differential accessibility of H1 sites at different stages of the cell cycle.

摘要

在哺乳动物细胞中,组蛋白H1上多达六个丝氨酸和苏氨酸在体内以细胞周期依赖性方式被磷酸化,这种方式长期以来一直与染色质凝聚相关联。与生长相关的H1激酶,现在被称为细胞周期蛋白依赖性激酶(CDK),被认为是负责这一过程的酶。本文描述了四种不同纯化的CDK对组蛋白H1的磷酸化作用。这四种CDK仅磷酸化H1的细胞周期特异性磷酸化位点,表明它们属于负责体内与生长相关的H1磷酸化的激酶类别。所有四种CDK都磷酸化所有间期和有丝分裂特异性的H1位点。除了(S/T)PXK共有磷酸化位点外,这四种CDK还磷酸化一个缺乏该序列的有丝分裂特异性体内H1磷酸化位点。这四种CDK中的任何一种在与生长相关的磷酸化位点之间都没有位点选择性,因为所有四种CDK都磷酸化所有相关位点。结果表明,体内观察到的细胞周期依赖性H1磷酸化必定涉及细胞周期不同阶段H1位点的不同可及性。

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