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首页> 外文期刊>Acta biomaterialia >Vascular differentiation of bone marrow stem cells is directed by a tunable three-dimensional matrix.
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Vascular differentiation of bone marrow stem cells is directed by a tunable three-dimensional matrix.

机译:骨髓干细胞的血管分化由可调节的三维矩阵控制。

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Microenvironmental cues are critical in regulating cell behavior and fate. The roles that matrix mechanical signals play in regulating cell behavior have recently been elucidated. An artificial matrix that can maintain the appropriate characteristics for transplanted stem cells is therefore needed to achieve a desired cell phenotype. The objective of this study was to develop a three-dimensional (3-D) matrix with tunable physical and mechanical properties and investigate their effects on mesenchymal stem cell (MSC) differentiation towards vascular cell types. In this study we developed an extracellular microenvironment by modifying fibrinogen with various polyethylene glycol (PEG) derivatives. We hypothesized that adjusting the type of PEG derivative to modify the resultant physical and mechanical characteristics of fibrin would allow us to create a tunable system for use in culture or in vivo in conjunction with a regenerative medicine strategy. Human MSC (hMSC) were entrapped into PEGylated fibrin matrices at a density of 50,000 cells ml(-1). Cell phenotypes were confirmed by immunofluorescent staining as well as the use of oligonucleotide arrays. Vascular phenotypes were correlated with measured mechanical properties and fiber diameters of the PEGylated fibrin matrices. Blocking studies were performed to identify mechanistic factors controlling MSC differentiation through selected blocking of matrix degradation or cell contraction. Cell-matrix interactions were also examined in vivo. Our results demonstrate that transdifferentiation of MSC towards an endothelial cell phenotype is profoundly affected by the 3-D matrix microenvironment. Our work provides a predictive road map for the creation of fibrin-based matrices that support robust endothelial cell gene expression and tubulogenesis.
机译:微环境提示对于调节细胞行为和命运至关重要。最近已经阐明了基质机械信号在调节细胞行为中的作用。因此,需要一种能够维持移植干细胞适当特性的人工基质,以实现所需的细胞表型。这项研究的目的是开发具有可调的物理和机械特性的三维(3-D)矩阵,并研究它们对间充质干细胞(MSC)向血管细胞类型分化的影响。在这项研究中,我们通过用各种聚乙二醇(PEG)衍生物修饰纤维蛋白原来开发细胞外微环境。我们假设调整PEG衍生物的类型以修饰纤维蛋白的物理和机械特性将使我们能够结合再生医学策略创建一个可用于培养或体内使用的可调系统。人类MSC(hMSC)以50,000个细胞ml(-1)的密度被包埋在PEG化纤维蛋白基质中。通过免疫荧光染色以及寡核苷酸阵列的使用来确认细胞表型。血管表型与聚乙二醇化纤维蛋白基质的机械性能和纤维直径相关。进行了阻断研究以鉴定通过选择的基质降解或细胞收缩阻断来控制MSC分化的机制因素。还在体内检查了细胞-基质的相互作用。我们的结果表明,MSC向内皮细胞表型的转分化受3-D基质微环境的影响很大。我们的工作为创建基于纤维蛋白的基质提供了可预测的路线图,这些基质支持强大的内皮细胞基因表达和肾小管生成。

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