Skeletal muscle-derived extracellular vesicles transport glycolytic enzymes to mediate muscle-to-bone crosstalk.

Shixing Ma, Xiaotao Xing, Haisen Huang, Xin Gao, Xun Xu, Jian Yang, Chengcheng Liao, Xuanhao Zhang, Jinglun Liu, Weidong Tian, Li Liao
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Abstract

Identification of cues originating from skeletal muscle that govern bone formation is essential for understanding the crosstalk between muscle and bone and for developing therapies for degenerative bone diseases. Here, we identified that skeletal muscle secreted multiple extracellular vesicles (Mu-EVs). These Mu-EVs traveled through the bloodstream to reach bone, where they were phagocytized by bone marrow mesenchymal stem/stromal cells (BMSCs). Mu-EVs promoted osteogenic differentiation of BMSCs and protected against disuse osteoporosis in mice. The quantity and bioactivity of Mu-EVs were tightly correlated with the function of skeletal muscle. Proteomic analysis revealed numerous proteins in Mu-EVs, some potentially regulating bone metabolism, especially glycolysis. Subsequent investigations indicated that Mu-EVs promoted the glycolysis of BMSCs by delivering lactate dehydrogenase A into these cells. In summary, these findings reveal that Mu-EVs play a vital role in BMSC metabolism regulation and bone formation stimulation, offering a promising approach for treating disuse osteoporosis.

骨骼肌衍生的细胞外小泡运输糖酵解酶以介导肌骨串扰。
识别源自骨骼肌的控制骨骼形成的线索对于理解肌肉和骨骼之间的串扰以及开发退行性骨病的治疗方法至关重要。在这里,我们发现骨骼肌分泌多个细胞外小泡(Mu-EVs)。这些Mu-EV通过血液到达骨骼,在那里它们被骨髓间充质干细胞/基质细胞(BMSC)吞噬。Mu-EVs促进BMSCs的成骨分化,并对小鼠废用性骨质疏松症具有保护作用。Mu-EVs的数量和生物活性与骨骼肌的功能密切相关。蛋白质组学分析显示Mu-EVs中有许多蛋白质,其中一些可能调节骨代谢,尤其是糖酵解。随后的研究表明,Mu-EVs通过将乳酸脱氢酶A输送到这些细胞中来促进BMSCs的糖酵解。总之,这些发现表明Mu-EVs在BMSC代谢调节和骨形成刺激中发挥着至关重要的作用,为治疗废用性骨质疏松症提供了一种有前景的方法。
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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