首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Lysyl 5-Hydroxylation a Novel Histone Modification by Jumonji Domain Containing 6 (JMJD6)
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Lysyl 5-Hydroxylation a Novel Histone Modification by Jumonji Domain Containing 6 (JMJD6)

机译:通过包含6(JMJD6)的Jumonji域进行的新型组蛋白修饰Lysyl 5-Hydroxylation

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摘要

JMJD6 is reported to hydroxylate lysyl residues of a splicing factor, U2AF65. In this study, we found that JMJD6 hydroxylates histone lysyl residues. In vitro experiments showed that JMJD6 has a binding affinity to histone proteins and hydroxylates multiple lysyl residues of histone H3 and H4 tails. Using JMJD6 knock-out mouse embryos, we revealed that JMJD6 hydroxylates lysyl residues of histones H2A/H2B and H3/H4 in vivo by amino acid composition analysis. 5-Hydroxylysine was detected at the highest level in histones purified from murine testis, which expressed JMJD6 at a significantly high level among various tissues examined, and JMJD6 overexpression increased the amount of 5-hydroxylysine in histones in human embryonic kidney 293 cells. These results indicate that histones are additional substrates of JMJD6 in vivo. Because 5-hydroxylation of lysyl residues inhibited N-acetylation and N-methylation by an acetyltransferase and a methyltransferase, respectively, in vitro, histone 5-hydroxylation may have important roles in epigenetic regulation of gene transcription or chromosomal rearrangement.
机译:据报道,JMJD6使剪接因子U2AF65的赖氨酰残基羟基化。在这项研究中,我们发现JMJD6将组蛋白赖氨酰残基羟基化。体外实验表明,JMJD6与组蛋白具有结合亲和力,可羟化组蛋白H3和H4尾部的多个赖氨酰残基。使用JMJD6敲除小鼠胚胎,我们揭示了JMJD6通过氨基酸组成分析在体内羟化组蛋白H2A / H2B和H3 / H4的赖氨酰残基。在从小鼠睾丸中纯化的组蛋白中检测到最高水平的5-羟赖氨酸,在所检查的各种组织中JMJD6的表达水平都很高,并且JMJD6的过表达增加了人胚肾293细胞中组蛋白中的5-羟赖氨酸的含量。这些结果表明,组蛋白是体内JMJD6的其他底物。因为赖氨酰残基的5-羟基化分别在体外通过乙酰转移酶和甲基转移酶抑制了N-乙酰化和N-甲基化,所以组蛋白5-羟基化可能在基因转录的表观遗传调控或染色体重排中起重要作用。

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