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JIL-1组蛋白H3S10激酶的羧基末端结构域与组蛋白H3相互作用,是正确靶向染色质所必需的。

The COOH-terminal domain of the JIL-1 histone H3S10 kinase interacts with histone H3 and is required for correct targeting to chromatin.

作者信息

Bao Xiaomin, Cai Weili, Deng Huai, Zhang Weiguo, Krencik Robert, Girton Jack, Johansen Jørgen, Johansen Kristen M

机构信息

Department of Biochemistry, Biophysics, and Molecular Biology, Iowa State University, Ames, Iowa 50011, USA.

出版信息

J Biol Chem. 2008 Nov 21;283(47):32741-50. doi: 10.1074/jbc.M806227200. Epub 2008 Sep 26.

Abstract

The JIL-1 histone H3S10 kinase in Drosophila localizes specifically to euchromatic interband regions of polytene chromosomes and is enriched 2-fold on the male X chromosome. JIL-1 can be divided into four main domains including an NH(2)-terminal domain, two separate kinase domains, and a COOH-terminal domain. Our results demonstrate that the COOH-terminal domain of JIL-1 is necessary and sufficient for correct chromosome targeting to autosomes but that both COOH- and NH(2)-terminal sequences are necessary for enrichment on the male X chromosome. We furthermore show that a small 53-amino acid region within the COOH-terminal domain can interact with the tail region of histone H3, suggesting that this interaction is necessary for the correct chromatin targeting of the JIL-1 kinase. Interestingly, our data indicate that the COOH-terminal domain alone is sufficient to rescue JIL-1 null mutant polytene chromosome defects including those of the male X chromosome. Nonetheless, we also found that a truncated JIL-1 protein which was without the COOH-terminal domain but retained histone H3S10 kinase activity was able to rescue autosome as well as partially rescue male X polytene chromosome morphology. Taken together these findings indicate that JIL-1 may participate in regulating chromatin structure by multiple and partially redundant mechanisms.

摘要

果蝇中的JIL-1组蛋白H3S10激酶特异性定位于多线染色体的常染色质间带区域,并且在雄性X染色体上富集两倍。JIL-1可分为四个主要结构域,包括一个NH(2)-末端结构域、两个独立的激酶结构域和一个COOH-末端结构域。我们的结果表明,JIL-1的COOH-末端结构域对于正确靶向常染色体是必要且充分的,但COOH-末端和NH(2)-末端序列对于在雄性X染色体上的富集都是必要的。我们还表明,COOH-末端结构域内一个53个氨基酸的小区域可以与组蛋白H3的尾部区域相互作用,这表明这种相互作用对于JIL-1激酶正确靶向染色质是必要的。有趣的是,我们的数据表明,单独的COOH-末端结构域足以挽救JIL-1缺失突变体的多线染色体缺陷,包括雄性X染色体的缺陷。尽管如此,我们还发现,一种截短的JIL-1蛋白,其没有COOH-末端结构域但保留了组蛋白H3S10激酶活性,能够挽救常染色体,并部分挽救雄性X多线染色体形态。综合这些发现表明,JIL-1可能通过多种部分冗余的机制参与调节染色质结构。

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