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The Role of SIRT6 Protein in Aging and Reprogramming of Human Induced Pluripotent Stem Cells

机译:SIRT6蛋白在人类诱导的多能干细胞老化和重编程中的作用

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摘要

Aging is known to be the single most important risk factor for multiple diseases. Sirtuin 6, or SIRT6, has recently been identified as a critical regulator of transcription, genome stability, telomere integrity, DNA repair, and metabolic homeostasis. A knockout mouse model of SIRT6 has displayed dramatic phenotypes of accelerated aging. In keeping with its role in aging, we demonstrated that human dermal fibroblasts (HDFs) from older human subjects were more resistant to reprogramming by classic Yamanaka factors than those from younger human subjects, but the addition of SIRT6 during reprogramming improved such efficiency in older HDFs substantially. Despite the importance of SIRT6, little is known about the molecular mechanism of its regulation. We show, for the first, time posttranscriptional regulation of SIRT6 by miR-766 and inverse correlation in the expression of this microRNA in HDFs from different age groups. Our results suggest that SIRT6 regulates miR-766 transcription via a feedback regulatory loop, which has implications for the modulation of SIRT6 expression in reprogramming of aging cells.
机译:已知衰老是多种疾病的最重要的单一危险因素。 Sirtuin 6或SIRT6最近被确定为转录,基因组稳定性,端粒完整性,DNA修复和代谢稳态的关键调节剂。 SIRT6的基因敲除小鼠模型显示出加速衰老的惊人表型。为了保持其在衰老中的作用,我们证明了来自较老人类受试者的人皮肤成纤维细胞(HDF)对经典Yamanaka因子的重编程比对较年轻人类受试者的抗性更高,但是在重编程过程中添加SIRT6可以改善在较老HDFs中的此类效率实质上。尽管SIRT6的重要性,对其调节的分子机制知之甚少。我们首先显示了miR-766对SIRT6的时间转录后调控,以及该microRNA在不同年龄组的HDF中的表达呈负相关。我们的结果表明,SIRT6通过反馈调节环调节miR-766转录,这对老化细胞的重编程中SIRT6表达的调节具有影响。

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