早产状况会改变肌肉干细胞及其生态位，导致肌肉再生和功能出现持久性损伤。

Preterm Birth Conditions Alter Muscle Stem Cells and Their Niche, Causing Lasting Impairments in Muscle Regeneration and Function.

作者信息

Deprez Alyson, Molina Thomas, Cagnone Gael, Garcia Pauline, Leclerc Séverine, Cloutier Anik, Desaulniers Rebecca, Ellezam Benjamin, Nuyt Anne Monique, Dumont Nicolas A

机构信息

CHU Sainte-Justine Azrieli Research Center, Montreal, Canada.

Faculty of Medicine, Department of Pharmacology and Physiology, Université de Montréal, Montreal, Canada.

出版信息

J Cachexia Sarcopenia Muscle. 2025 Oct;16(5):e70058. doi: 10.1002/jcsm.70058.

DOI:10.1002/jcsm.70058

PMID:40955870

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12439181/

Abstract

BACKGROUND

Preterm birth-related conditions affect the development of multiple organs, such as the heart, the lungs and the brain, leading to long-term alterations in their function and a higher risk of comorbidities. Emerging evidence also indicates that the skeletal muscles are affected. We aimed to understand the mechanisms underlying these changes in skeletal muscles.

METHODS

A rodent model of transient neonatal hyperoxia and muscle samples of human babies born at term or preterm were used to investigate the impact of preterm birth-related conditions on muscle stem cells, the engine of muscle growth and repair. Single cell transcriptomics, in vitro culture of myoblasts or single myofibres, ex vivo muscle contractile properties and in vivo experiments (cardiotoxin-induced muscle injury) were performed to determine the impact of preterm birth on muscle stem cell function and regenerative capacity.

RESULTS

Preterm birth-related conditions reduced the muscle stem cell pool from the newborn stage (-30%, p = 0.0134) until adulthood (-56%, p < 0.0001), along with impaired myogenic capacity and regenerative potential. In vitro analysis from rats showed impaired self-renewal and reduced myotube size (-28.8%, p = 0.004). Human samples suggest a similar trend towards smaller myotube size in muscle stem cells from infants born at the earlier gestational age. Single-cell RNA-seq on rat samples revealed an enriched TNF-α/NF-κB signalling pathway within subsets of muscle stem cells. This pathway, mediated in part by interaction with macrophages, influences muscle stem cell fate decisions and myogenic trajectories. Culture experiments showed that myotubes treated with conditioned medium from macrophages of rats exposed to hyperoxia have reduced diameters (-66.5%, p = 0.0216). Early administration of an inhibitor of TNF-α (Infliximab) restored the muscle stem cell pool postinjury (63%, p = 0.0073) and regenerative capacity.

CONCLUSIONS

Overall, preterm birth-related conditions promote an inflammatory microenvironment that disrupts the muscle stem cell pool and their function. This mechanism could explain the muscle atrophy and weakness observed in individuals born preterm and suggests potential therapeutic strategies to improve overall health outcomes in this population.

摘要

背景

早产相关情况会影响多个器官的发育，如心脏、肺和大脑，导致其功能长期改变以及患合并症的风险增加。新出现的证据还表明骨骼肌也会受到影响。我们旨在了解骨骼肌这些变化背后的机制。

方法

使用新生鼠短暂高氧模型以及足月或早产出生的人类婴儿的肌肉样本，来研究早产相关情况对肌肉干细胞（肌肉生长和修复的动力源）的影响。进行了单细胞转录组学、成肌细胞或单根肌纤维的体外培养、离体肌肉收缩特性以及体内实验（心脏毒素诱导的肌肉损伤），以确定早产对肌肉干细胞功能和再生能力的影响。

结果

早产相关情况使肌肉干细胞库从新生儿期就开始减少（减少30%，p = 0.0134），直至成年期（减少56%，p < 0.0001），同时成肌能力和再生潜力受损。对大鼠的体外分析显示自我更新受损且肌管大小减小（减少28.8%，p = 0.004）。人类样本表明，胎龄较小的婴儿的肌肉干细胞中肌管大小也有类似的变小趋势。对大鼠样本进行的单细胞RNA测序显示，在肌肉干细胞亚群中肿瘤坏死因子-α/核因子-κB信号通路富集。该通路部分通过与巨噬细胞相互作用介导，影响肌肉干细胞的命运决定和成肌轨迹。培养实验表明，用暴露于高氧环境的大鼠巨噬细胞的条件培养基处理的肌管直径减小（减少66.5%，p = 0.0216）。早期给予肿瘤坏死因子-α抑制剂（英夫利昔单抗）可在损伤后恢复肌肉干细胞库（恢复63%，p = 0.0073）及其再生能力。