Epigenetic traits inscribed in chromatin accessibility in aged hematopoietic stem cells

Naoki Itokawa(Chiba University), Motohiko Oshima(The University of Tokyo), Shuhei Koide(The University of Tokyo), Naoya Takayama(Chiba University), Wakako Kuribayashi(Chiba University), Yaeko Nakajima‐Takagi(The University of Tokyo), Kazumasa Aoyama(Chiba University), Satoshi Yamazaki(University of Tsukuba), Kiyoshi Yamaguchi(The University of Tokyo), Yoichi Furukawa(The University of Tokyo), Koji Eto(Chiba University), Atsushi Iwama(Chiba University)
Nature Communications
May 16, 2022
Cited by 85Open Access
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Abstract

Hematopoietic stem cells (HSCs) exhibit considerable cell-intrinsic changes with age. Here, we present an integrated analysis of transcriptome and chromatin accessibility of aged HSCs and downstream progenitors. Alterations in chromatin accessibility preferentially take place in HSCs with aging, which gradually resolve with differentiation. Differentially open accessible regions (open DARs) in aged HSCs are enriched for enhancers and show enrichment of binding motifs of the STAT, ATF, and CNC family transcription factors that are activated in response to external stresses. Genes linked to open DARs show significantly higher levels of basal expression and their expression reaches significantly higher peaks after cytokine stimulation in aged HSCs than in young HSCs, suggesting that open DARs contribute to augmented transcriptional responses under stress conditions. However, a short-term stress challenge that mimics infection is not sufficient to induce persistent chromatin accessibility changes in young HSCs. These results indicate that the ongoing and/or history of exposure to external stresses may be epigenetically inscribed in HSCs to augment their responses to external stimuli.


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