Mohri Yasuaki, Nie Jialiang, Morinaga Hironobu, Kato Tomoki, Aoto Takahiro, Yamanashi Takashi, Nanba Daisuke, Matsumura Hiroyuki, Kirino Sakura, Kobiyama Kouji, Ishii Ken J, Hayashi Masahiro, Suzuki Tamio, Namiki Takeshi, Seita Jun, Nishimura Emi K
Division of Aging and Regeneration, The Institute of Medical Science, The University of Tokyo, Tokyo, Japan.
Department of Stem Cell Biology, Medical Research Institute, Tokyo Medical and Dental University, presently the Institute of Science Tokyo, Tokyo, Japan.
Nat Cell Biol. 2025 Oct;27(10):1647-1659. doi: 10.1038/s41556-025-01769-9. Epub 2025 Oct 6.
The exposome, an individual's lifelong environmental exposure, profoundly impacts health. Somatic tissues undergo functional decline with age, exhibiting characteristic ageing phenotypes, including hair greying and cancer. However, the specific genotoxins, signals and cellular mechanisms underlying each phenotype remain largely unknown. Here we report that melanocyte stem cells (McSCs) and their niche coordinately determine individual stem cell fate through antagonistic, stress-responsive pathways, depending on the type of genotoxic damage incurred. McSC fate tracking in mice revealed that McSCs undergo cellular senescence-coupled differentiation (seno-differentiation) in response to DNA double-strand breaks, resulting in their selective depletion and hair greying, and effectively protecting against melanoma. Conversely, carcinogens can suppress McSC seno-differentiation, even in cells harbouring double-strand breaks, by activating arachidonic acid metabolism and the niche-derived KIT ligand, thereby promoting McSC self-renewal. Collectively, the fate of individual stem cell clones-expansion versus exhaustion-cumulatively and antagonistically governs ageing phenotypes through interaction with the niche.
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