依赖于 NAD+ 的代谢检查点调节造血干细胞的活化和衰老。

IF 17 Q1 CELL BIOLOGY Nature aging Pub Date : 2024-07-23 DOI:10.1038/s43587-024-00670-8
Zehan Song, Sang Hee Park, Wei-Chieh Mu, Yufan Feng, Chih-Ling Wang, Yifei Wang, Marine Barthez, Ayane Maruichi, Jiayue Guo, Fanghan Yang, Anita Wong Lin, Kartoosh Heydari, Claudia C. S. Chini, Eduardo N. Chini, Cholsoon Jang, Danica Chen
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摘要

造血干细胞(HSCs)如何在整个生命周期内维持代谢平衡以支持组织修复和再生,目前尚无定论。在这里,我们发现,CD38是一种依赖于NAD+的代谢酶,在年轻小鼠体内通过诱导线粒体Ca2+流入和线粒体代谢促进造血干细胞增殖。相反,由于 NAD+ 代谢失调和线粒体应激管理受损,衰老过程中 CD38 的异常上调是老年小鼠造血干细胞退化的驱动因素。线粒体钙离子通道是线粒体 Ca2+ 流入的介质,它也支持年轻小鼠的造血干细胞增殖,但却驱动着老年小鼠造血干细胞的衰退。药物灭活 CD38 可逆转造血干细胞的衰老和衰老小鼠造血系统的病理生理变化。总之,我们的研究强调了一个 NAD+ 代谢检查点,它能平衡线粒体激活以支持造血干细胞增殖和线粒体应激管理以增强造血干细胞在整个生命周期的自我更新,并将异常 Ca2+ 信号传导与造血干细胞衰老联系起来。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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An NAD+-dependent metabolic checkpoint regulates hematopoietic stem cell activation and aging
How hematopoietic stem cells (HSCs) maintain metabolic homeostasis to support tissue repair and regeneration throughout the lifespan is elusive. Here, we show that CD38, an NAD+-dependent metabolic enzyme, promotes HSC proliferation by inducing mitochondrial Ca2+ influx and mitochondrial metabolism in young mice. Conversely, aberrant CD38 upregulation during aging is a driver of HSC deterioration in aged mice due to dysregulated NAD+ metabolism and compromised mitochondrial stress management. The mitochondrial calcium uniporter, a mediator of mitochondrial Ca2+ influx, also supports HSC proliferation in young mice yet drives HSC decline in aged mice. Pharmacological inactivation of CD38 reverses HSC aging and the pathophysiological changes of the aging hematopoietic system in aged mice. Together, our study highlights an NAD+ metabolic checkpoint that balances mitochondrial activation to support HSC proliferation and mitochondrial stress management to enhance HSC self-renewal throughout the lifespan, and links aberrant Ca2+ signaling to HSC aging. Song et al. show that in young mice CD38 supports hematopoietic stem cell (HSC) proliferation by regulating Ca2+ signaling and mitochondrial activity. Conversely, the upregulation of CD38 during aging causes dysregulation of NAD metabolism, mitochondrial stress and HSC dysfunction.
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