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通过控制细胞形状,由 3D 支架结构决定干细胞命运。

The determination of stem cell fate by 3D scaffold structures through the control of cell shape.

机构信息

Polymers Division, National Institute of Standards & Technology, Gaithersburg, MD 20899, USA.

出版信息

Biomaterials. 2011 Dec;32(35):9188-96. doi: 10.1016/j.biomaterials.2011.08.054. Epub 2011 Sep 3.

Abstract

Stem cell response to a library of scaffolds with varied 3D structures was investigated. Microarray screening revealed that each type of scaffold structure induced a unique gene expression signature in primary human bone marrow stromal cells (hBMSCs). Hierarchical cluster analysis showed that treatments sorted by scaffold structure and not by polymer chemistry suggesting that scaffold structure was more influential than scaffold composition. Further, the effects of scaffold structure on hBMSC function were mediated by cell shape. Of all the scaffolds tested, only scaffolds with a nanofibrous morphology were able to drive the hBMSCs down an osteogenic lineage in the absence of osteogenic supplements. Nanofiber scaffolds forced the hBMSCs to assume an elongated, highly branched morphology. This same morphology was seen in osteogenic controls where hBMSCs were cultured on flat polymer films in the presence of osteogenic supplements (OS). In contrast, hBMSCs cultured on flat polymer films in the absence of OS assumed a more rounded and less-branched morphology. These results indicate that cells are more sensitive to scaffold structure than previously appreciated and suggest that scaffold efficacy can be optimized by tailoring the scaffold structure to force cells into morphologies that direct them to differentiate down the desired lineage.

摘要

研究了具有不同 3D 结构的支架文库对干细胞的反应。微阵列筛选显示,每种支架结构都在原代人骨髓基质细胞(hBMSCs)中诱导出独特的基因表达特征。层次聚类分析表明,处理结果是根据支架结构而不是聚合物化学分类的,这表明支架结构比支架组成更具影响力。此外,支架结构对 hBMSC 功能的影响是通过细胞形状介导的。在所测试的所有支架中,只有具有纳米纤维形态的支架能够在没有成骨补充剂的情况下将 hBMSCs 沿着成骨谱系驱动。纳米纤维支架迫使 hBMSCs 呈现出拉长的、高度分支的形态。在成骨对照中也观察到了相同的形态,其中 hBMSCs 在存在成骨补充剂的情况下在聚合物薄膜上培养(OS)。相比之下,在没有 OS 的情况下在聚合物薄膜上培养的 hBMSCs 则呈现出更圆和分支较少的形态。这些结果表明,细胞对支架结构的敏感性比以前认识到的要高得多,并表明通过将支架结构调整为迫使细胞形成引导其沿着所需谱系分化的形态,可以优化支架的功效。

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