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Adult equine bone-marrow stromal cells produce a cartilage-like ECM superior to animal-matched adult chondrocytes

机译:成体马骨髓基质细胞产生软骨样ECm,优于动物匹配的成体软骨细胞

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摘要

Our objective was to evaluate the age-dependent mechanical phenotype of bone marrow stromal cell- (BMSC-) and chondrocyte-produced cartilage-like neo-tissue and to elucidate the matrix-associated mechanisms which generate this phenotype. Cells from both immature (2–4 month-old foals) and skeletally-mature (2–5 year-old adults) mixed-breed horses were isolated from animal-matched bone marrow and cartilage tissue, encapsulated in self-assembling-peptide hydrogels, and cultured with and without TGF-β1 supplementation. BMSCs and chondrocytes from both donor ages were encapsulated with high viability. BMSCs from both ages produced neo-tissue with higher mechanical stiffness than that produced by either young or adult chondrocytes. Young, but not adult, chondrocytes proliferated in response to TGF-β1 while BMSCs from both age groups proliferated with TGF-β1. Young chondrocytes stimulated by TGF-β1 accumulated ECM with 10-fold higher sulfated-glycosaminoglycan content than adult chondrocytes and 2–3-fold higher than BMSCs of either age. The opposite trend was observed for hydroxyproline content, with BMSCs accumulating 2–3-fold more than chondrocytes, independent of age. Size-exclusion chromatography of extracted proteoglycans showed that an aggrecan-like peak was the predominant sulfated proteoglycan for all cell types. Direct measurement of aggrecan core protein length and chondroitin sulfate chain length by single molecule atomic force microscopy imaging revealed that, independent of age, BMSCs produced longer core protein and longer chondroitin sulfate chains, and fewer short core protein molecules than chondrocytes, suggesting that the BMSC-produced aggrecan has a phenotype more characteristic of young tissue than chondrocyte-produced aggrecan. Aggrecan ultrastructure, ECM composition, and cellular proliferation combine to suggest a mechanism by which BMSCs produce a superior cartilage-like neo-tissue than either young or adult chondrocytes.
机译:我们的目的是评估年龄依赖性的骨髓基质细胞(BMSC)和软骨细胞产生的软骨样新组织的机械表型,并阐明产生该表型的基质相关机制。从与动物匹配的骨髓和软骨组织中分离出未成熟的(2-4月龄的小马驹)和骨骼成熟的(2-5岁的成年马)细胞,并封装在自组装肽水凝胶中,并在有和没有TGF-β1的情况下进行培养。来自两个供体年龄的BMSC和软骨细胞都被高存活率封装。两个年龄的骨髓间充质干细胞产生的新组织均具有比年轻或成年软骨细胞更高的机械刚度。青年人而非成年软骨细胞对TGF-β1有反应,而这两个年龄段的BMSC均由TGF-β1引起。 TGF-β1刺激的年轻软骨细胞积累的ECM的硫酸化糖胺聚糖含量比成人软骨细胞高10倍,比任何年龄的BMSC高2-3倍。羟脯氨酸含量的变化趋势相反,而与年龄无关,BMSC的积聚比软骨细胞多2-3倍。提取的蛋白聚糖的尺寸排阻色谱分析表明,聚集蛋白样峰是所有细胞类型的主要硫酸化蛋白聚糖。通过单分子原子力显微镜成像直接测量聚集蛋白聚糖核心蛋白长度和硫酸软骨素链长度,发现与年龄无关,BMSCs比软骨细胞产生更长的核心蛋白和更长的硫酸软骨素链,以及更少的短核心蛋白分子,这表明BMSC产生的聚集蛋白聚糖具有比软骨细胞产生的聚集蛋白聚糖更年轻的组织的表型。 Aggrecan的超微结构,ECM组成和细胞增殖相结合,提示一种机制,使BMSC产生比年轻或成年软骨细胞更好的软骨样新组织。

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