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内源性细胞外基质增强了人骨髓间充质干细胞的聚集形成和存活。

Endogenous extracellular matrices enhance human mesenchymal stem cell aggregate formation and survival.

机构信息

Dept. of Chemical and Biomedical Engineering, Florida State University, Tallahassee, FL 32310, USA.

出版信息

Biotechnol Prog. 2013 Mar-Apr;29(2):441-51. doi: 10.1002/btpr.1686. Epub 2013 Mar 1.

DOI:10.1002/btpr.1686
PMID:23296993
Abstract

Human mesenchymal stem or stromal cell (hMSC) therapies have promise across a wide range of diseases. However, inefficient cell delivery and low cell survival at injury sites reduce efficacy and are the major barriers in hMSC-based therapy. Formation of three-dimensional (3D) hMSC aggregates has been found to activate hMSC functions from enhancing secretion of therapeutic factors for improving cell migration and survival. As the stromal cells in bone marrow, hMSCs are significant sources of extracellular matrix (ECM) proteins and growth factors, which form an interactive microenvironment to influence hMSC fate via paracrine and autocrine actions. To date, however, the impact of the extracellular microenvironment on hMSC properties in the aggregates remains unknown. In the present study, we investigated the role of endogenous ECM matrices on hMSC aggregate formation and survival under ischemic stress. The results demonstrated that the preservation of endogenous ECM in the aggregates formed by thermal lifting (termed TLAs) as opposed to the aggregates formed by enzymatically detached hMSCs (termed EDAs) enhanced cell proliferation, multilineage potential, and survival under ischemic stress. The improved cell proliferation and viability in the TLAs is attributed to the incorporation of endogenous ECM proteins in the TLAs and their promitotic and antioxidant properties. The results demonstrate a novel method for the formation of hMSC aggregates via thermal responsive surface and highlight the significant contribution of the ECM in preserving hMSC properties in the 3D aggregates.

摘要

人源间充质干细胞或基质细胞 (hMSC) 疗法在多种疾病中具有广阔的应用前景。然而,细胞在损伤部位的递送效率低和存活率低,降低了疗效,这是 hMSC 治疗的主要障碍。三维 (3D) hMSC 聚集体的形成已被发现可激活 hMSC 功能,增强治疗因子的分泌,从而促进细胞迁移和存活。作为骨髓中的基质细胞,hMSCs 是细胞外基质 (ECM) 蛋白和生长因子的重要来源,这些蛋白和生长因子形成一个相互作用的微环境,通过旁分泌和自分泌作用影响 hMSC 的命运。然而,迄今为止,细胞外微环境对聚集体中 hMSC 特性的影响仍不清楚。在本研究中,我们研究了内源性 ECM 基质在 hMSC 聚集体形成和缺血应激下存活中的作用。结果表明,与通过酶分离 hMSC 形成的聚集体(称为 EDAs)相比,热提升形成的聚集体(称为 TLAs)中内源性 ECM 的保留增强了细胞增殖、多能性和在缺血应激下的存活。TLAs 中内源性 ECM 蛋白的掺入及其促进细胞增殖和抗氧化特性是细胞增殖和活力提高的原因。该结果证明了通过热响应表面形成 hMSC 聚集体的新方法,并强调了 ECM 在保持 3D 聚集体中 hMSC 特性方面的重要贡献。

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