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A reduction in CD90 (THY-1) expression results in increased differentiation of mesenchymal stromal cells

机译:CD90(THY-1)表达的减少导致间充质基质细胞的分化增加

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Background Mesenchymal stromal cells (MSCs) are multipotent progenitor cells used in several cell therapies. MSCs are characterized by the expression of CD73, CD90, and CD105 cell markers, and the absence of CD34, CD45, CD11a, CD19, and HLA-DR cell markers. CD90 is a glycoprotein present in the MSC membranes and also in adult cells and cancer stem cells. The role of CD90 in MSCs remains unknown. Here, we sought to analyse the role that CD90 plays in the characteristic properties of in vitro expanded human MSCs. Methods We investigated the function of CD90 with regard to morphology, proliferation rate, suppression of T-cell proliferation, and osteogenic/adipogenic differentiation of MSCs by reducing the expression of this marker using CD90-target small hairpin RNA lentiviral vectors. Results The present study shows that a reduction in CD90 expression enhances the osteogenic and adipogenic differentiation of MSCs in vitro and, unexpectedly, causes a decrease in CD44 and CD166 expression. Conclusion Our study suggests that CD90 controls the differentiation of MSCs by acting as an obstacle in the pathway of differentiation commitment. This may be overcome in the presence of the correct differentiation stimuli, supporting the idea that CD90 level manipulation may lead to more efficient differentiation rates in vitro.
机译:背景间充质基质细胞(MSCs)是用于多种细胞疗法的多能祖细胞。 MSCs的特征在于CD73,CD90和CD105细胞标志物的表达,以及不存在CD34,CD45,CD11a,CD19和HLA-DR细胞标志物。 CD90是存在于MSC膜以及成体细胞和癌症干细胞中的一种糖蛋白。 CD90在MSC中的作用仍然未知。在这里,我们试图分析CD90在体外扩增人MSCs的特征中所起的作用。方法我们通过使用靶向CD90的小发夹RNA慢病毒载体降低该标志物的表达,研究了CD90在形态,增殖速率,T细胞增殖抑制和成骨/成脂分化方面的功能。结果本研究表明,CD90表达的降低可增强MSC在体外的成骨和成脂分化,并出乎意料地引起CD44和CD166表达的降低。结论我们的研究表明CD90通过充当分化承诺途径的障碍来控制MSC的分化。在存在正确的分化刺激的情况下可以克服这一点,从而支持CD90水平操纵可导致更有效的体外分化率的观点。

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