Department of Molecular, Cellular and Developmental Biology, University of Colorado, Boulder, CO 80309, USA.
BioFrontiers Institute, University of Colorado, Boulder, 3415 Colorado Avenue, Boulder, CO 80303, USA.
Stem Cell Reports. 2023 Jun 13;18(6):1325-1339. doi: 10.1016/j.stemcr.2023.05.005.
Skeletal muscle function and regenerative capacity decline during aging, yet factors driving these changes are incompletely understood. Muscle regeneration requires temporally coordinated transcriptional programs to drive myogenic stem cells to activate, proliferate, fuse to form myofibers, and to mature as myonuclei, restoring muscle function after injury. We assessed global changes in myogenic transcription programs distinguishing muscle regeneration in aged mice from young mice by comparing pseudotime trajectories from single-nucleus RNA sequencing of myogenic nuclei. Aging-specific differences in coordinating myogenic transcription programs necessary for restoring muscle function occur following muscle injury, likely contributing to compromised regeneration in aged mice. Differences in pseudotime alignment of myogenic nuclei when comparing aged with young mice via dynamic time warping revealed pseudotemporal differences becoming progressively more severe as regeneration proceeds. Disruptions in timing of myogenic gene expression programs may contribute to incomplete skeletal muscle regeneration and declines in muscle function as organisms age.
骨骼肌功能和再生能力随着衰老而下降,但导致这些变化的因素尚不完全清楚。肌肉再生需要时间协调的转录程序来驱动成肌干细胞激活、增殖、融合形成肌纤维,并成熟为肌核,在损伤后恢复肌肉功能。我们通过比较肌核的单细胞 RNA 测序的伪时间轨迹,评估了区分老年小鼠和年轻小鼠肌肉再生的成肌转录程序的全局变化。肌肉损伤后,发生了恢复肌肉功能所必需的协调成肌转录程序的衰老特异性差异,这可能导致老年小鼠的再生受损。通过动态时间规整比较老年和年轻小鼠的肌核伪时对齐时,发现随着再生的进行,伪时差异变得越来越严重。成肌基因表达程序时间的中断可能导致不完全的骨骼肌再生和肌肉功能下降,随着生物体的衰老。
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