转录组重编程筛选鉴定SRSF1为返老还童因子

Alexandru M Plesa, Sascha Jung, Helen H Wang, Fawad Omar, Michael Shadpour, David Choy Buentello, Maria C Perez-Matos, Naftali Horwitz, George Cai, Zhen-Kai Ngian, Carol V de Magalhaes, Amy J Wagers, William B Mair, Antonio del Sol Mesa, George M Church
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摘要

衰老是一个复杂的过程,表现为生物系统随时间变化的功能衰退。表观遗传和转录组谱的年龄相关变化已成功用于测量衰老过程1,2。此外,通过干预(如诱导Yamanaka因子)调节基因调控网络已被证明可以逆转衰老特征并改善细胞功能3,4。然而,这种干预在体内返老还老方面存在安全性和有效性限制5,6,强调需要确定新的年龄逆转因素。在这里,我们发现SRSF1是一种新的年轻化因子,可以在体外和体内改善细胞功能。利用cDNA过表达筛选和转录组读数,我们发现SRSF1诱导将细胞转录组重编程为更年轻的状态。此外,我们观察到SRSF1过表达对衰老、蛋白酶体功能、胶原生成和ROS应激的有益变化。最后,我们发现SRSF1可以促进体外和体内伤口愈合,并与生物体寿命有关。我们的研究为使用转录组重编程筛选发现年龄逆转干预提供了概念证明,并确定SRSF1是细胞年轻化的有希望的靶标。
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Transcriptomic reprogramming screen identifies SRSF1 as rejuvenation factor
Aging is a complex process that manifests through the time-dependent functional decline of a biological system. Age-related changes in epigenetic and transcriptomic profiles have been successfully used to measure the aging process 1,2 . Moreover, modulating gene regulatory networks through interventions such as the induction of the Yamanaka factors has been shown to reverse aging signatures and improve cell function 3,4 . However, this intervention has safety and efficacy limitations for in vivo rejuvenation 5,6 , underscoring the need for identifying novel age reversal factors. Here, we discovered SRSF1 as a new rejuvenation factor that can improve cellular function in vitro and in vivo . Using a cDNA overexpression screen with a transcriptomic readout we identified that SRSF1 induction reprograms the cell transcriptome towards a younger state. Furthermore, we observed beneficial changes in senescence, proteasome function, collagen production, and ROS stress upon SRSF1 overexpression. Lastly, we showed that SRSF1 can improve wound healing in vitro and in vivo and is linked to organismal longevity. Our study provides a proof of concept for using transcriptomic reprogramming screens in the discovery of age reversal interventions and identifies SRSF1 as a promising target for cellular rejuvenation.
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