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ETS1 acts as a regulator of human healthy aging via decreasing ribosomal activity

Fu‐Hui Xiao, Qin Yu, Zhili Deng, Ke Yang, Yunshuang Ye, Ming‐Xia Ge, Dongjing Yan, Haotian Wang, Xiao‐Qiong Chen, Liqin Yang, Bin-Yu Yang, Rong Lin, Wen Zhang, Xing‐Li Yang, Lei Dong, Yonghan He, Jumin Zhou, Wangwei Cai, Ji Li, Qing‐Peng Kong

2022Science Advances63 citationsDOIOpen Access PDF

Abstract

Adaptation to reduced energy production during aging is a fundamental issue for maintaining healthspan or prolonging life span. Currently, however, the underlying mechanism in long-lived people remains poorly understood. Here, we analyzed transcriptomes of 185 long-lived individuals (LLIs) and 86 spouses of their children from two independent Chinese longevity cohorts and found that the ribosome pathway was significantly down-regulated in LLIs. We found that the down-regulation is likely controlled by ETS1 (ETS proto-oncogene 1), a transcription factor down-regulated in LLIs and positively coexpressed with most ribosomal protein genes (RPGs). Functional assays showed that ETS1 can bind to RPG promoters, while ETS1 knockdown reduces RPG expression and alleviates cellular senescence in human dermal fibroblast (HDF) and embryonic lung fibroblast (IMR-90) cells. As protein synthesis/turnover in ribosomes is an energy-intensive cellular process, the decline in ribosomal biogenesis governed by ETS1 in certain female LLIs may serve as an alternative mechanism to achieve energy-saving and healthy aging.

Topics & Concepts

Ribosome biogenesisGene knockdownETS1BiologyTranscription factorRibosomal proteinRibosomeSenescenceCell biologyTranscriptomeTranscription (linguistics)GeneticsGeneGene expressionRNALinguisticsPhilosophyRNA modifications and cancerGenomics and Chromatin DynamicsDNA Repair Mechanisms
ETS1 acts as a regulator of human healthy aging via decreasing ribosomal activity | Litcius