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多切变微装置中间质干细胞和软骨细胞的命运受 Yes 相关蛋白调节。

Mesenchymal stem cell and chondrocyte fates in a multishear microdevice are regulated by Yes-associated protein.

机构信息

Department of Orthopaedics, First Affiliated Hospital of Dalian Medical University, Dalian, PR China.

出版信息

Stem Cells Dev. 2013 Jul 15;22(14):2083-93. doi: 10.1089/scd.2012.0685. Epub 2013 Apr 5.

DOI:10.1089/scd.2012.0685
PMID:23442010
Abstract

Mechanical cues exert considerable influence on the fates of stem cells and terminally differentiated chondrocytes. The elucidation of the interactions between cell fate and mechanical cues in nuclear mechanotransduction will provide new clues to modulate tissue homeostasis and regeneration. In this study, we used an integrated microfluidic perfusion device to simultaneously generate multiple-parameter fluid shear stresses to investigate the role of fluid flow stimuli in the regulation of Yes-associated protein (YAP) expression and the fates of mesenchymal stem cells (MSCs) and primary chondrocytes. YAP expression was regulated by the level of fluid flow stimulus in both MSCs and chondrocytes. An increase in the magnitude of stimulation enhanced the expression of YAP, ultimately resulting in an increase in osteogenesis and a decrease in adipogenesis for MSCs, and initiating dedifferentiation for chondrocytes. Cytochalasin D not only repressed nuclear YAP accumulation in the flow state, but also abrogated flow-induced effects on MSC differentiation and the chondrocyte phenotype, resulting in MSC adipogenesis and the maintenance of the chondrocyte phenotype. Our findings reveal the connection between YAP and MSC/chondrocyte fates in a fluid flow-induced mechanical microenvironment and provide new insights into the mechanisms by which mechanical cues regulate the fates of MSCs and chondrocytes.

摘要

力学刺激对干细胞和终末分化的软骨细胞的命运有很大的影响。阐明核机械转导中细胞命运与力学刺激之间的相互作用,将为调节组织稳态和再生提供新的线索。在本研究中,我们使用集成的微流控灌注装置来同时产生多种参数的流体剪切应力,以研究流体流动刺激在调节 Yes 相关蛋白 (YAP) 表达和间充质干细胞 (MSCs) 和原代软骨细胞命运中的作用。在 MSC 和软骨细胞中,YAP 的表达受流体流动刺激水平的调节。刺激幅度的增加增强了 YAP 的表达,最终导致 MSC 的成骨增加和脂肪形成减少,以及软骨细胞的去分化。细胞松弛素 D 不仅抑制了流动状态下核 YAP 的积累,而且消除了对 MSC 分化和软骨细胞表型的流动诱导作用,导致 MSC 脂肪形成和维持软骨细胞表型。我们的发现揭示了在流体流动诱导的力学微环境中 YAP 与 MSC/软骨细胞命运之间的联系,并为机械刺激调节 MSC 和软骨细胞命运的机制提供了新的见解。

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