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The role of bFGF on the ability of MSC to activate endogenous regenerative mechanisms in an ectopic bone formation model

机译:bFGF对异位骨形成模型中MSC激活内源性再生机制能力的作用

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The view depicting bone marrow (BM)-derived mesenchymal stem cells (MSC) as a uniform population differentiating into new-tissue builder cells is evolving toward the concept of a heterogeneous population of stem/progenitor cells secreting bioactive molecules, and contributing to establish an on-site regenerative microenvironment. We report that in an ectopic bone formation model the intrinsic MSC capability to activate endogenous regenerative mechanisms is critically dependent on the commitment level of implanted MSC. We demonstrate that the presence of bFGF in the culture medium during mouse MSC expansion invitro is the key factor for the selection of subpopulations inducing host regenerative responses. We developed a novel strategy combining SILAC-LC-MS/MS quantitative proteomics of conditioned culture media and gene expression profiling to disentangle the major role of MSC in modulating the microenvironment toward the damage resolution. The correspondence between results provided by the applied techniques proved that the most statistically significant biological processes favored by the bFGF treatment were carried out by secreted factors. In particular, the immune response, the inflammatory response, the response to wounding and chemotaxis were all upregulated in bFGF-selected MSC. We propose these processes as majorly involved in activating the endogenous responses triggered by trophic effects of implanted bFGF-selected MSC.
机译:将骨髓(BM)来源的间充质干细胞(MSC)描述为分化为新组织构建细胞的统一群体的观点正在朝着分泌生物活性分子的干/祖细胞异质群体的概念发展,并有助于建立一种现场再生微环境。我们报告说,在异位骨形成模型中,内在的MSC激活内源性再生机制的能力关键取决于植入的MSC的承诺水平。我们证明在小鼠MSC体外扩增过程中培养基中bFGF的存在是选择诱导宿主再生反应的亚群的关键因素。我们开发了一种新的策略,将条件培养基的SILAC-LC-MS / MS定量蛋白质组学与基因表达谱相结合,以解开MSC在调节微环境中朝着损害解决的主要作用。应用技术提供的结果之间的对应关系证明,bFGF治疗支持的最具有统计学意义的生物学过程是由分泌因子进行的。特别地,在bFGF选择的MSC中,免疫应答,炎性应答,对伤口和趋化性的应答均被上调。我们提出这些过程主要参与激活由植入bFGF选择的MSC的营养作用触发的内源性反应。

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