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滑膜干细胞及其对微纤维支架多孔性的反应。

Synovial stem cells and their responses to the porosity of microfibrous scaffold.

机构信息

UC Berkeley-UCSF Graduate Program in Bioengineering, Berkeley, CA 94720, USA.

出版信息

Acta Biomater. 2013 Jul;9(7):7264-75. doi: 10.1016/j.actbio.2013.03.009. Epub 2013 Mar 19.

Abstract

Tissue-specific stem cells can be coaxed or harvested for tissue regeneration. In this study, we identified and characterized a new type of stem cells from the synovial membrane of knee joint, named neural crest cell-like synovial stem cells (NCCL-SSCs). NCCL-SSCs showed the characteristics of neural crest stem cells: they expressed markers such as Sox10, Sox17 and S100β, were clonable, and could differentiate into neural lineages as well as mesenchymal lineages, although NCCL-SSCs were not derived from neural crest during the development. When treated with transforming growth factor β1 (TGF-β1), NCCL-SSCs differentiated into mesenchymal stem cells (MSCs), lost the expression of Sox17 and the differentiation potential into neural lineages, but retained the potential of differentiating into mesenchymal lineages. To determine the responses of NCCL-SSCs to microfibrous scaffolds for tissue engineering, electrospun composite scaffolds with various porosities were fabricated by co-electrospinning of structural and sacrificial microfibers. The increase in the porosity in microfibrous scaffolds enhanced cell infiltration in vitro and in vivo, but did not affect the morphology and the proliferation of NCCL-SSCs. Interestingly, microfibrous scaffolds with higher porosity increased the expression of chondrogenic and osteogenic genes but suppressed smooth muscle and adipogenic genes. These results suggest that the differentiation of NCCL-SSCs can be controlled by both soluble chemical factors and biophysical factors such as the porosity of the scaffold. Engineering both NCCL-SSCs and scaffolds will have tremendous potential for tissue regeneration.

摘要

组织特异性干细胞可以被诱导或采集用于组织再生。在这项研究中,我们从膝关节滑膜中鉴定和表征了一种新型干细胞,命名为神经嵴细胞样滑膜干细胞(NCCL-SSCs)。NCCL-SSCs 表现出神经嵴干细胞的特征:它们表达 Sox10、Sox17 和 S100β 等标志物,具有克隆性,并能分化为神经谱系和间充质谱系,尽管 NCCL-SSCs 在发育过程中并非来自神经嵴。当用转化生长因子β1(TGF-β1)处理时,NCCL-SSCs 分化为间充质干细胞(MSCs),失去 Sox17 的表达和向神经谱系分化的潜力,但保留向间充质谱系分化的潜力。为了确定 NCCL-SSCs 对组织工程微纤维支架的反应,通过结构和牺牲微纤维的共电纺制备了具有不同孔隙率的复合电纺支架。微纤维支架中孔隙率的增加增强了细胞在体外和体内的渗透,但不影响 NCCL-SSCs 的形态和增殖。有趣的是,具有更高孔隙率的微纤维支架增加了软骨和成骨基因的表达,但抑制了平滑肌和成脂基因的表达。这些结果表明,NCCL-SSCs 的分化可以通过可溶性化学因子和生物物理因子(如支架的孔隙率)共同控制。工程化 NCCL-SSCs 和支架将为组织再生带来巨大潜力。

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