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首页> 外文期刊>Osteoarthritis and cartilage >Comparison of the catabolic effects of fibronectin fragments in human knee and ankle cartilages.
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Comparison of the catabolic effects of fibronectin fragments in human knee and ankle cartilages.

机译:纤连蛋白片段对人的膝盖和踝关节软骨的分解代谢作用的比较。

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OBJECTIVE: To compare the response of knee and ankle cartilages to fibronectin fragments (Fn-f) in terms of kinetics of matrix proteoglycan (PG) degradation and synthesis, since previous data had shown that knee was more sensitive to Fn-f in terms of steady-state PG content. DESIGN: Human knee and ankle cartilage explants were treated with the 29kDa Fn-f, and its effects on PG-degradation kinetics, on the half-lives of 35S-sulfate-labeled PG, on PG synthesis suppression and on matrix metalloproteinase -3 (MMP-3) were compared. Cultures were also treated with the interleukin (IL) receptor antagonist protein (IRAP) in order to determine whether IL-1 is involved in the Fn-f effect. RESULTS: The Fn-f enhanced PG-degradation rates in both human knee and ankle cartilages. Knee cartilage showed a greater effect of Fn-f on half-lives of newly synthesized 35S-labeled PG than ankle. The extent of release of MMP-3 was similar for human ankle and knee cartilages. However, PG synthesis in knee cartilage was sensitive to 10- to 100-fold lower concentrations of Fn-f than was ankle cartilage. IRAP partially reversed Fn-f activity in ankle cartilages. CONCLUSIONS: The role of Fn-f in proteolysis leading to cartilage damage appears to be minor in human cartilages than had previously been shown for bovine. This decreased proteolysis is true for both knee and ankle. The major difference between human ankle and knee cartilage appears to be greater sensitivity to PG synthesis suppression in knee cartilage. A further indication that IL-1 is involved in the pathway was provided by the partial reversal with IRAP.
机译:目的:根据基质蛋白聚糖(PG)降解和合成的动力学,比较膝关节和踝关节软骨对纤连蛋白片段(Fn-f)的反应,因为先前的数据表明,膝关节对Fn-f的敏感性更高。稳态PG含量。设计:用29kDa Fn-f处理人的膝盖和踝关节软骨外植体,它对PG降解动力学,35S硫酸盐标记的PG的半衰期,PG的合成抑制和基质金属蛋白酶-3(比较了MMP-3)。还用白介素(IL)受体拮抗剂蛋白(IRAP)处理培养物,以确定IL-1是否参与Fn-f效应。结果:Fn-f提高了人类膝盖和踝关节软骨的PG降解率。膝盖软骨显示Fn-f对新合成的35S标记的PG的半衰期的影响大于踝关节。 MMP-3的释放程度与人类脚踝和膝盖软骨相似。但是,与软骨相比,膝关节软骨中PG的合成对Fn-f浓度低10至100倍敏感。 IRAP部分逆转了脚踝软骨中的Fn-f活动。结论:Fn-f在蛋白水解中导致软骨损伤的作用在人软骨中似乎比以前对牛的作用要小。这种降低的蛋白水解作用对膝盖和脚踝都是正确的。人脚踝和膝盖软骨之间的主要差异似乎是对抑制膝盖软骨中PG合成的敏感性更高。 IRAP的部分逆转提供了IL-1参与该途径的进一步指示。

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