Restraining Lysosomal Activity Preserves Hematopoietic Stem Cell Quiescence and Potency

抑制溶酶体活性可维持造血干细胞的静止状态和分化潜能

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作者:Raymond Liang ,Tasleem Arif ,Svetlana Kalmykova ,Artem Kasianov ,Miao Lin ,Vijay Menon ,Jiajing Qiu ,Jeffrey M Bernitz ,Kateri Moore ,Fangming Lin ,Deanna L Benson ,Nikolaos Tzavaras ,Milind Mahajan ,Dmitri Papatsenko ,Saghi Ghaffari

Abstract

Quiescence is a fundamental property that maintains hematopoietic stem cell (HSC) potency throughout life. Quiescent HSCs are thought to rely on glycolysis for their energy, but the overall metabolic properties of HSCs remain elusive. Using combined approaches, including single-cell RNA sequencing (RNA-seq), we show that mitochondrial membrane potential (MMP) distinguishes quiescent from cycling-primed HSCs. We found that primed, but not quiescent, HSCs relied readily on glycolysis. Notably, in vivo inhibition of glycolysis enhanced the competitive repopulation ability of primed HSCs. We further show that HSC quiescence is maintained by an abundance of large lysosomes. Repression of lysosomal activation in HSCs led to further enlargement of lysosomes while suppressing glucose uptake. This also induced increased lysosomal sequestration of mitochondria and enhanced the competitive repopulation ability of primed HSCs by over 90-fold in vivo. These findings show that restraining lysosomal activity preserves HSC quiescence and potency and may be therapeutically relevant.

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