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透明质酸的添加可提高细胞浸润,并促进基于胶原的软骨组织工程支架中的早期软骨分化。

Addition of hyaluronic acid improves cellular infiltration and promotes early-stage chondrogenesis in a collagen-based scaffold for cartilage tissue engineering.

机构信息

Department of Anatomy, Royal College of Surgeons in Ireland, 123 St. Stephens Green, Dublin 2, Ireland.

出版信息

J Mech Behav Biomed Mater. 2012 Jul;11:41-52. doi: 10.1016/j.jmbbm.2011.11.012. Epub 2011 Dec 6.

DOI:10.1016/j.jmbbm.2011.11.012
PMID:22658153
Abstract

The response of mesenchymal stem cells (MSCs) to a matrix largely depends on the composition as well as the extrinsic mechanical and morphological properties of the substrate to which they adhere to. Collagen-glycosaminoglycan (CG) scaffolds have been extensively used in a range of tissue engineering applications with great success. This is due in part to the presence of the glycosaminoglycans (GAGs) in complementing the biofunctionality of collagen. In this context, the overall goal of this study was to investigate the effect of two GAG types: chondroitin sulphate (CS) and hyaluronic acid (HyA) on the mechanical and morphological characteristics of collagen-based scaffolds and subsequently on the differentiation of rat MSCs in vitro. Morphological characterisation revealed that the incorporation of HyA resulted in a significant reduction in scaffold mean pore size (93.9 μm) relative to collagen-CS (CCS) scaffolds (136.2 μm). In addition, the collagen-HyA (CHyA) scaffolds exhibited greater levels of MSC infiltration in comparison to the CCS scaffolds. Moreover, these CHyA scaffolds showed significant acceleration of early stage gene expression of SOX-9 (approximately 60-fold higher, p<0.01) and collagen type II (approximately 35-fold higher, p<0.01) as well as cartilage matrix production (7-fold higher sGAG content) in comparison to CCS scaffolds by day 14. Combining their ability to stimulate MSC migration and chondrogenesis in vitro, these CHyA scaffolds show great potential as appropriate matrices for promoting cartilage tissue repair.

摘要

间充质干细胞 (MSCs) 对基质的反应在很大程度上取决于基质的组成以及其附着的基质的外在机械和形态特性。胶原糖胺聚糖 (CG) 支架已广泛应用于多种组织工程应用,并取得了巨大成功。这部分归因于糖胺聚糖 (GAGs) 的存在,补充了胶原的生物功能。在这种情况下,本研究的总体目标是研究两种 GAG 类型:硫酸软骨素 (CS) 和透明质酸 (HyA) 对基于胶原的支架的机械和形态特性的影响,以及随后对体外大鼠 MSCs 分化的影响。形态特征表明,与胶原-硫酸软骨素 (CCS) 支架 (136.2 μm) 相比,透明质酸 (HyA) 的掺入导致支架平均孔径显著减小 (93.9 μm)。此外,与 CCS 支架相比,胶原蛋白-透明质酸 (CHyA) 支架表现出更高水平的 MSC 渗透。此外,与 CCS 支架相比,这些 CHyA 支架在早期基因表达 SOX-9(约 60 倍,p<0.01)和 II 型胶原(约 35 倍,p<0.01)以及软骨基质产生(sGAG 含量高 7 倍)方面表现出显著的加速作用到第 14 天。这些 CHyA 支架在体外具有刺激 MSC 迁移和成软骨的能力,因此具有促进软骨组织修复的巨大潜力。

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