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胶原基整合素 α 和 α 介导的信号对三维环境下人骨髓间充质干细胞成骨的影响。

Influence of collagen-based integrin α and α mediated signaling on human mesenchymal stem cell osteogenesis in three dimensional contexts.

机构信息

Center for Biotechnology and Interdisciplinary Studies, Rensselaer Polytechnic Institute, Troy, New York, 12180.

Institute of Biosciences and Technology, Texas A&M University System Health Science Center, Houston, Texas, 77030-3303.

出版信息

J Biomed Mater Res A. 2018 Oct;106(10):2594-2604. doi: 10.1002/jbm.a.36451. Epub 2018 Sep 8.

Abstract

Collagen I interactions with integrins α and α are known to support human mesenchymal stem cell (hMSC) osteogenesis. Nonetheless, elucidating the relative impact of specific integrin interactions has proven challenging, in part due to the complexity of native collagen. In the present work, we employed two collagen-mimetic proteins-Scl2-2 and Scl2-3- to compare the osteogenic effects of integrin α versus α signaling. Scl2-2 and Scl2-3 were both derived from Scl2-1, a triple helical protein lacking known cell adhesion, cytokine binding, and matrix metalloproteinase sites. However, Scl2-2 and Scl2-3 were each engineered to display distinct collagen-based cell adhesion motifs: GFPGER (binding integrins α and α ) or GFPGEN (binding only integrin α ), respectively. hMSCs were cultured within poly(ethylene glycol) (PEG) hydrogels containing either Scl2-2 or Scl2-3 for 2 weeks. PEG-Scl2-2 gels were associated with increased hMSC osterix expression, osteopontin production, and calcium deposition relative to PEG-Scl2-3 gels. These data indicate that integrin α signaling may have an increased osteogenic effect relative to integrin α . Since p38 is activated by integrin α but not by integrin α , hMSCs were further cultured in PEG-Scl2-2 hydrogels in the presence of a p38 inhibitor. Results suggest that p38 activity may play a key role in collagen-supported hMSC osteogenesis. This knowledge can be used toward the rational design of scaffolds which intrinsically promote hMSC osteogenesis. © 2018 Wiley Periodicals, Inc. J Biomed Mater Res Part A: 106A: 2594-2604, 2018.

摘要

I 型胶原蛋白与整合素 α 和 α 的相互作用已被证实可支持人骨髓间充质干细胞(hMSC)的成骨作用。尽管如此,阐明特定整合素相互作用的相对影响具有一定的挑战性,部分原因是天然胶原蛋白的复杂性。在本研究中,我们使用了两种胶原蛋白模拟蛋白-Scl2-2 和 Scl2-3-来比较整合素 α 与 α 信号对成骨的影响。Scl2-2 和 Scl2-3 均源自 Scl2-1,这是一种缺乏已知细胞黏附、细胞因子结合和基质金属蛋白酶结合位点的三螺旋蛋白。然而,Scl2-2 和 Scl2-3 都经过了工程设计,分别显示出独特的基于胶原蛋白的细胞黏附基序:GFPGER(结合整合素 α 和 α )或 GFPGEN(仅结合整合素 α )。hMSC 在含有 Scl2-2 或 Scl2-3 的聚乙二醇(PEG)水凝胶中培养 2 周。与 PEG-Scl2-3 凝胶相比,PEG-Scl2-2 凝胶与 hMSC osterix 表达、骨桥蛋白产生和钙沉积的增加相关。这些数据表明,与整合素 α 相比,整合素 α 信号可能具有更强的成骨作用。由于 p38 被整合素 α 而不是整合素 α 激活,因此 hMSC 进一步在含有 p38 抑制剂的 PEG-Scl2-2 水凝胶中培养。结果表明,p38 活性可能在胶原蛋白支持的 hMSC 成骨中起关键作用。这些知识可用于合理设计内在促进 hMSC 成骨的支架。2018 年 Wiley 期刊公司。J 生物医学材料研究 A 部分:106A:2594-2604,2018 年。

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