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Study of the microRNA expression profile of foreskin derived mesenchymal stromal cells following inflammation priming

机译:炎症引发后包皮来源的间充质基质细胞的microRNA表达谱研究

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摘要

BackgroundDue to their self-renewal capacity, multi-lineage potential, and immunomodulatory properties, mesenchymal stromal cells (MSCs) are an attractive tool for different therapeutic strategies. Foreskin (FSK), considered as a biological waste material, has already been shown to be a valuable source of MSCs. Besides their typical fibroblast like morphology and International Society for cellular Therapy compliant phenotype, foreskin-MSCs (FSK–MSCs) are clonogenic, and highly proliferative cells with multi-lineage and strong immunomodulatory capacities. Of importance, FSK–MSCs properly adjust their fate following exposure to inflammatory signals. Being potent regulators of gene expression, miRNAs are involved in modulating nearly all cellular processes and in orchestrating the roles of different immune cells. In this study, we characterized the miRNome of FSK–MSCs by determining the expression profile of 380 different miRNAs in inflammation primed vs. control non-primed cells.
机译:背景由于间充质基质细胞(MSC)的自我更新能力,多谱系潜能和免疫调节特性,因此它们是用于不同治疗策略的诱人工具。包皮(FSK)被认为是一种生物废料,已被证明是MSC的重要来源。除了其典型的成纤维细胞形态和国际细胞疗法顺应性表型外,包皮MSCs(FSK–MSCs)具有克隆性,并且是高度增殖的细胞,具有多种谱系和强大的免疫调节能力。重要的是,FSK–MSC在暴露于炎症信号后可以适当地调整其命运。作为基因表达的有效调节剂,miRNA参与调节几乎所有细胞过程以及协调不同免疫细胞的作用。在这项研究中,我们通过确定380种不同miRNA在炎症引发与对照未引发细胞中的表达谱来表征FSK–MSC的miRNome。

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