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SPR-5 is a histone H3K4 demethylase with a role in meiotic double-strand break repair

机译:SPR-5是一种组蛋白H3K4脱甲基酶,在减数分裂双链断裂修复中起作用

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摘要

Regulation of histone methylation levels has long been implicated in multiple cellular processes, many of which involve transcription. Here, however, we report a unique role for the Caenorhabditis elegans histone demethylase SPR-5 in meiotic DNA double-strand break repair (DSBR). SPR-5 shows enzymatic activity toward H3K4me2 both in vitro and in the nematode germline, and spr-5 mutants show several phenotypes indicating a perturbation of DSBR, including increased p53-dependent germ cell apoptasis, increased levels of the DSBR marker RAD-51, and sensitivity toward DSB-inducing treatments. spr-S mutants show no transcriptional misregulation of known DSBR involved genes. Instead, SPR-5 shows a rapid subcellular relocalization upon DSB-inducing treatment, which suggests that SPR-5 may function directly in DSBR.
机译:长期以来,组蛋白甲基化水平的调节涉及多个细胞过程,其中许多过程涉及转录。但是,在这里,我们报道了秀丽隐杆线虫组蛋白脱甲基酶SPR-5在减数分裂DNA双链断裂修复(DSBR)中的独特作用。 SPR-5在体外和线虫种系中均表现出对H3K4me2的酶活性,spr-5突变体显示出几种表型,表明DSBR受到干扰,包括增加的p53依赖性生殖细胞凋亡,DSBR标记RAD-51的水平升高,对DSB诱导治疗的敏感性。 spr-S突变体未显示已知DSBR参与基因的转录失调。相反,SPR-5在诱导DSB后显示出快速的亚细胞再定位,这表明SPR-5可能直接在DSBR中起作用。

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