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Inhibition of histone acetyltransferase GCN5 extends lifespan in both yeast and human cell lines

机译:组蛋白乙酰转移酶GCN5对酵母和人细胞系中的寿命延伸

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Histone acetyltransferases (HATs) are important enzymes that transfer acetyl groups onto histones and thereby regulate both gene expression and chromosomal structures. Previous work has shown that the activation of sirtuins, which are histone deacetylases, can extend lifespan. This suggests that inhibiting HATs may have a similar beneficial effect. In the present study, we utilized a range of HAT inhibitors or heterozygous Gcn5 and Ngg1 mutants to demonstrate marked yeast life extension. In human cell lines, HAT inhibitors and selective RNAi‐mediated Gcn5 or Ngg1 knockdown reduced the levels of aging markers and promoted proliferation in senescent cells. Furthermore, this observed lifespan extension was associated with the acetylation of histone H3 rather than that of H4. Specifically, it was dependent upon H3K9Ac and H3K18Ac modifications. We also found that the ability of caloric restriction to prolong lifespan is Gcn5‐, Ngg1‐, H3K9‐, and H3K18‐dependent. Transcriptome analysis revealed that these changes were similar to those associated with heat shock and were inversely correlated with the gene expression profiles of aged yeast and aged worms. Through a bioinformatic analysis, we also found that HAT inhibition activated subtelomeric genes in human cell lines. Together, our results suggest that inhibiting the HAT Gcn5 may be an effective means of increasing longevity.
机译:组蛋白乙酰转移酶(帽子)是将乙酰基转移到组蛋白上的重要酶,从而调节两个基因表达和染色体结构。以前的工作表明,SIRTUIN的激活,即组蛋白脱乙酰酶,可以延长寿命。这表明抑制帽子可能具有类似的有益效果。在本研究中,我们利用一系列帽抑制剂或杂合GCN5和NGG1突变体来证明标记的酵母生命延伸。在人细胞系中,帽抑制剂和选择性RNAi介导的GCN5或NGG1敲低降低了衰老标志物的水平并促进了衰老细胞的增殖。此外,这种观察到的寿命延伸与组蛋白H3的乙酰化而不是H4的乙酰化相关。具体而言,它取决于H3K9AC和H3K18AC的修饰。我们还发现,热量限制延长寿命的能力为GCN5,NGG1,H3K9-和H3K18依赖性。转录组分析表明,这些变化与与热休克相关的变化类似,与老年酵母和老化蠕虫的基因表达谱相关。通过生物信息分析,我们还发现帽子抑制活性的人细胞系中的亚细胞胶质基因。我们的结果表明,抑制帽GCN5可能是增加寿命的有效手段。

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