Transcriptomic analysis of skeletal muscle regeneration across mouse lifespan identifies altered stem cell states.

IF 17 Q1 CELL BIOLOGY

Nature aging Pub Date : 2024-11-22 DOI:10.1038/s43587-024-00756-3

Lauren D Walter, Jessica L Orton, Ioannis Ntekas, Ern Hwei Hannah Fong, Viviana I Maymi, Brian D Rudd, Iwijn De Vlaminck, Jennifer H Elisseeff, Benjamin D Cosgrove

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Abstract

In aging, skeletal muscle regeneration declines due to alterations in both myogenic and non-myogenic cells and their interactions. This regenerative dysfunction is not understood comprehensively or with high spatiotemporal resolution. We collected an integrated atlas of 273,923 single-cell transcriptomes and high-resolution spatial transcriptomic maps from muscles of young, old and geriatric mice (~5, 20 and 26 months old) at multiple time points following myotoxin injury. We identified eight immune cell types that displayed accelerated or delayed dynamics by age. We observed muscle stem cell states and trajectories specific to old and geriatric muscles and evaluated their association with senescence by scoring experimentally derived and curated gene signatures in both single-cell and spatial transcriptomic data. This revealed an elevation of senescent-like muscle stem cell subsets within injury zones uniquely in aged muscles. This Resource provides a holistic portrait of the altered cellular states underlying muscle regenerative decline across mouse lifespan.

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跨小鼠寿命的骨骼肌再生转录组分析确定了干细胞状态的改变。

在衰老过程中，由于成肌细胞和非成肌细胞及其相互作用的改变，骨骼肌再生能力下降。这种再生功能障碍尚未得到全面或高时空分辨率的了解。我们在肌毒素损伤后的多个时间点从年轻、年老和老年小鼠（约 5 个月、20 个月和 26 个月）的肌肉中收集了 273,923 个单细胞转录组的综合图集和高分辨率空间转录组图。我们确定了八种免疫细胞类型，它们在不同年龄段表现出加速或延迟的动态变化。我们观察了老年肌肉和老年肌肉特有的肌肉干细胞状态和轨迹，并通过对单细胞和空间转录组数据中实验得出的和策划的基因特征进行评分，评估了它们与衰老的关联。这揭示了老年肌肉损伤区内类似衰老的肌肉干细胞亚群的增加。该资源为小鼠整个生命周期中肌肉再生能力衰退的细胞状态变化提供了整体描述。

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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来源期刊

Nature aging

CiteScore

14.70

自引率

0.00%

发文量