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Mitotic Histone H3 Phosphorylation by Vaccinia-Related Kinase 1 in Mammalian Cells

机译:牛痘相关激酶1在哺乳动物细胞中的有丝分裂组蛋白H3磷酸化。

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摘要

Mitotic chromatin condensation is essential for cell division in eukaryotes. Posttranslational modification of the N-terminal tail of histone proteins, particularly by phosphorylation by mitotic histone kinases, may facilitate this process. In mammals, aurora B is believed to be the mitotic histone H3 Ser10 kinase; however, it is not sufficient to phosphorylate H3 Ser10 with aurora B alone. We show that histone H3 is phosphorylated by vaccinia-related kinase 1 (VRK1). Direct phosphorylation of Thr3 and Ser10 in H3 by VRK1 both in vitro and in vivo was observed. Loss of VRK1 activity was associated with a marked decrease in H3 phosphorylation during mitosis. Phosphorylation of Ser10 by VRK1 is similar to that by aurora B. Moreover, expression and chromatin localization of VRK1 depended on the cell cycle phase. Overexpression of VRK1 resulted in a dramatic condensation of nuclei. Our findings collectively support a role of VRK1 as a novel mitotic histone H3 kinase in mammals.
机译:有丝分裂染色质凝聚对于真核生物的细胞分裂至关重要。组蛋白蛋白质N末端尾部的翻译后修饰,特别是通过有丝分裂组蛋白激酶的磷酸化,可能会促进这一过程。在哺乳动物中,极光B被认为是有丝分裂组蛋白H3 Ser10激酶。然而,仅用极光B磷酸化H3 Ser10是不够的。我们显示,组蛋白H3被牛痘相关激酶1(VRK1)磷酸化。在体外和体内均观察到VRK1在H3中将Thr3和Ser10直接磷酸化。 VRK1活性的丧失与有丝分裂期间H3磷酸化的明显降低有关。 VRK1对Ser10的磷酸化与极光B相似。此外,VRK1的表达和染色质定位取决于细胞周期阶段。 VRK1的过表达导致细胞核急剧凝结。我们的发现共同支持了VRK1作为哺乳动物中新的有丝分裂组蛋白H3激酶的作用。

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