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Muscle-Specific Histone H3K36 Dimethyltransferase SET-18 Shortens Lifespan of Caenorhabditis elegans by Repressing daf-16a Expression

机译:特定于肌肉的组蛋白H3K36二甲基转移酶SET-18通过抑制daf-16a表达缩短秀丽线虫的寿命。

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Summary Mounting evidence shows that histone methylation, a typical epigenetic mark, is crucial for gene expression regulation during aging. Decreased trimethylation of Lys 36 on histone H3 (H3K36me3) in worms and yeast is reported to shorten lifespan. The function of H3K36me2 in aging remains unclear. In this study, we identified Caenorhabditis elegans SET-18 as a histone H3K36 dimethyltransferase. SET-18 deletion extended lifespan and increased oxidative stress resistance, dependent on daf-16 activity in the insulin/IGF pathway. In set-18 mutants, transcription of daf-16 isoform a ( daf-16a ) was specifically upregulated. Accordingly, a decrease in H3K36me2 on daf-16a promoter was observed. Muscle-specific expression of SET-18 increased in aged worms (day 7 and day 11), attributable to elevation of global H3K36me2 and inhibition of daf-16a expression. Consequently, longevity was shortened. These findings suggested that chromatic repression mediated by tissue-specific H3K36 dimethyltransferase might be detrimental to lifespan and may have implications in human age-related diseases.
机译:总结越来越多的证据表明,组蛋白甲基化是一种典型的表观遗传标记,对于衰老过程中的基因表达调控至关重要。据报道,蠕虫和酵母中组蛋白H3(H3K36me3)上Lys 36的三甲基化降低,会缩短寿命。 H3K36me2在衰老中的功能仍然不清楚。在这项研究中,我们确定秀丽隐杆线虫SET-18是组蛋白H3K36二甲基转移酶。 SET-18缺失可延长寿命并增加抗氧化应激性,具体取决于胰岛素/ IGF途径中的daf-16活性。在set-18突变体中,daf-16亚型a(daf-16a)的转录被特异上调。因此,观察到daf-16a启动子上的H3K36me2减少。 SET-18的肌肉特异性表达在衰老的蠕虫中(第7天和第11天)增加,这归因于整体H3K36me2的升高和daf-16a表达的抑制。因此,寿命缩短。这些发现表明,由组织特异性H3K36二甲基转移酶介导的色阻可能对寿命有害,并且可能与人类年龄相关疾病有关。

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