In vivo partial reprogramming alters age-associated molecular changes during physiological aging in mice

重编程 衰老 KLF4公司 生物 表观遗传学 转录组 SOX2 表型 细胞生物学 基因表达 遗传学 胚胎干细胞 基因
作者
Kristen Browder,Pradeep Reddy,Mako Yamamoto,Amin Haghani,Isabel Guillen,Sanjeeb Kumar Sahu,Chao Wang,Yosu Luque,Javier Prieto,Lei Shi,Kensaku Shojima,Tomoaki Hishida,Zijuan Lai,Qingling Li,Feroza K. Choudhury,Weng Ruh Wong,Yuxin Liang,Dewakar Sangaraju,Wendy Sandoval,Concepción Rodrı́guez Esteban
出处
期刊:Nature Aging 卷期号:2 (3): 243-253 被引量:209
标识
DOI:10.1038/s43587-022-00183-2
摘要

Partial reprogramming by expression of reprogramming factors (Oct4, Sox2, Klf4 and c-Myc) for short periods of time restores a youthful epigenetic signature to aging cells and extends the life span of a premature aging mouse model. However, the effects of longer-term partial reprogramming in physiologically aging wild-type mice are unknown. Here, we performed various long-term partial reprogramming regimens, including different onset timings, during physiological aging. Long-term partial reprogramming lead to rejuvenating effects in different tissues, such as the kidney and skin, and at the organismal level; duration of the treatment determined the extent of the beneficial effects. The rejuvenating effects were associated with a reversion of the epigenetic clock and metabolic and transcriptomic changes, including reduced expression of genes involved in the inflammation, senescence and stress response pathways. Overall, our observations indicate that partial reprogramming protocols can be designed to be safe and effective in preventing age-related physiological changes. We further conclude that longer-term partial reprogramming regimens are more effective in delaying aging phenotypes than short-term reprogramming.
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