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Controlling the fate of regenerative cells with engineered platelet-derived extracellular vesicles

机译:控制再生细胞的命运工程血小板源细胞外囊泡

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Extracellular vesicles (EVs) have emerged as cell-free nanotherapeutic agents for the potential treatment of multiple diseases and for tissue engineering and regenerative medicine strategies. Nevertheless, the field has typically relied on EVs derived from stem cells, the production of which in high quantities and high reproducibility is still under debate. Platelet-derived EVs were produced by a freeze–thaw method of platelet concentrates, a highly available clinical waste material. The aim of this study was to produce and thoroughly characterize platelet-derived EVs and understand their effects in adipose-tissue derived stem cells (hASCs), endothelial cells (HUVECs) and macrophages. Two different EV populations were obtained after differential centrifugation, namely small EVs (sEVs) and medium EVs (mEVs), which showed different size distributions and unique proteomic signatures. EV interaction with hASCs resulted in the modulation of the gene expression of markers related to their commitment toward different lineages. Moreover, mEVs showed higher angiogenic potential than sEVs, in a tube formation assay with HUVECs. Also, the EVs were able to modulate macrophage polarization. Altogether, these results suggest that platelet-derived EVs are promising candidates to be used as biochemical signals or therapeutic tools in tissue engineering and regenerative medicine approaches.
机译:细胞外囊泡(EVs)已成为nanotherapeutic游离代理的潜在的多种疾病和治疗组织工程和再生医学策略。依靠EVs来源于干细胞生产的高数量和高再现性仍在争论。血小板源电动汽车产生的血小板浓缩液的冻融方法高可用性临床废物。本研究旨在生产和彻底描述血小板源EVs和理解他们在脂肪组织衍生干细胞的影响细胞(hASCs), (HUVECs)和内皮细胞巨噬细胞。获得了差速离心后,即小型电动车(股票)和中型电动汽车(兆电子伏),显示不同的分布和大小吗独特的蛋白质组签名。hASCs导致基因的调制表达式相关的标记他们的承诺对不同的血统。血管生成可能高于股票,在管形成和HUVECs化验。能够调节巨噬细胞极化。总之,这些结果表明,血小板源电动汽车是有希望的候选人用作生化信号或治疗工具在组织工程和再生医学方法。

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