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Novel SCRG1/BST1 axis regulates self-renewal, migration, and osteogenic differentiation potential in mesenchymal stem cells

机译:新型SCRG1 / BST1轴调节间充质干细胞的自我更新,迁移和成骨分化潜能

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Human mesenchymal stem cells (hMSCs) remodel or regenerate various tissues through several mechanisms. Here, we identified the hMSC-secreted protein SCRG1 and its receptor BST1 as a positive regulator of self-renewal, migration, and osteogenic differentiation. SCRG1 and BST1 gene expression decreased during osteogenic differentiation of hMSCs. Intriguingly, SCRG1 maintained stem cell marker expression (Oct-4 and CD271/LNGFR) and the potentials of self-renewal, migration, and osteogenic differentiation, even at high passage numbers. Thus, the novel SCRG1/BST1 axis determines the fate of hMSCs by regulating their kinetic and differentiation potentials. Our findings provide a new perspective on methods for ex vivo expansion of hMSCs that maintain native stem cell potentials for bone-forming cell therapy.
机译:人间充质干细胞(hMSCs)通过几种机制重塑或再生各种组织。在这里,我们确定了hMSC分泌的蛋白SCRG1及其受体BST1是自我更新,迁移和成骨分化的积极调节剂。 hMSCs成骨分化过程中,SCRG1和BST1基因表达降低。有趣的是,即使在高传代数下,SCRG1仍能维持干细胞标志物的表达(Oct-4和CD271 / LNGFR)以及自我更新,迁移和成骨分化的潜力。因此,新型的SCRG1 / BST1轴通过调节hMSC的动力学和分化潜能来决定其命运。我们的发现为hMSCs的体外扩增方法提供了新的视角,该方法可保持天然干细胞潜力用于成骨细胞治疗。

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