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首页> 外文期刊>Arthritis and Rheumatism >Osteoarthritic synovial tissue inhibition of proteoglycan production in human osteoarthritic knee cartilage: establishment and characterization of a long-term cartilage-synovium coculture.
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Osteoarthritic synovial tissue inhibition of proteoglycan production in human osteoarthritic knee cartilage: establishment and characterization of a long-term cartilage-synovium coculture.

机译:骨关节炎滑膜组织抑制人骨关节炎膝软骨蛋白多糖的产生:长期软骨-滑膜联合培养的建立和表征。

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OBJECTIVE: Although both cartilage and synovium are affected in osteoarthritis (OA), no in vitro coculture models of human OA tissue have been described. The aim of this study was to develop an in vitro model that includes both the synovium and cartilage of patients with knee OA. METHODS: Explants of human OA cartilage and synovium were cultured alone or in coculture for 21 days. Histologic evaluation and analyses of lactate dehydrogenase release, matrix metalloproteinase (MMP) activity, content, release, and synthesis of glycosaminoglycan (GAG), and cytokine production were used to evaluate synovial tissue functionality and its effect on cartilage metabolism. To assess the possibility of intervention in the model system, the effect of triamcinolone was studied. RESULTS: Throughout the entire culture period, OA synovial tissue remained viable and produced cytokines. Monocultures of synovial and cartilage explants produced different cytokine subsets, with the subsets found in coculture being most similar to those previously described in OA synovial fluid. MMP activity was detectable only in the synovial explant monoculture and in coculture. Cocultures showed a reduction in final GAG content (P < 0.02), attributable to an inhibition of GAG production (P < 0.001) rather than an increase in GAG release. Addition of triamcinolone inhibited cytokine production and MMP activity in coculture and synovial tissue monoculture and counteracted the inhibition of GAG production induced by coculture. In cartilage monoculture, however, triamcinolone reduced GAG production. CONCLUSION: OA synovium affects cartilage metabolism by reducting GAG production. Triamcinolone can relieve this effect of synovial tissue, while being inhibitory when added to cartilage monoculture. These results clearly indicate the importance of tissue coculture as a promising tool for studying OA pathophysiology and for development of possible interventions.
机译:目的:尽管软骨和滑膜均受骨关节炎(OA)的影响,但尚未描述人OA组织的体外共培养模型。这项研究的目的是建立一个包括膝骨关节炎患者的滑膜和软骨在内的体外模型。方法:将人OA软骨和滑膜外植体单独培养或共培养21天。组织学评估和乳酸脱氢酶释放,基质金属蛋白酶(MMP)活性,糖胺聚糖(GAG)的含量,释放和合成,以及细胞因子的产生,用于评估滑膜组织功能及其对软骨代谢的影响。为了评估干预模型系统的可能性,研究了曲安西龙的作用。结果:在整个培养过程中,OA滑膜组织保持活力并产生细胞因子。滑膜和软骨外植体的单培养产生不同的细胞因子亚群,共培养中发现的亚群与先前在OA滑液中描述的亚群最相似。 MMP活性仅在滑膜外植体单培养和共培养中可检测到。共培养显示最终GAG含量降低(P <0.02),这归因于GAG产生的抑制(P <0.001),而不是GAG释放的增加。加入曲安奈德可抑制共培养和滑膜组织单培养中细胞因子的产生和MMP活性,并抵消了共培养诱导的GAG产生的抑制作用。然而,在软骨单一培养中,曲安西龙减少了GAG的产生。结论:OA滑膜通过减少GAG的产生影响软骨的代谢。曲安西龙可以减轻滑膜组织的这种作用,而在加入软骨单一培养物中时具有抑制作用。这些结果清楚地表明,组织共培养作为研究OA病理生理学和开发可能的干预措施的有前途工具的重要性。

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