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首页> 外文期刊>Inflammation research: Official journal of the European Histamine Research Society >Novel selective MMP-13 inhibitors reduce collagen degradation in bovine articular and human osteoarthritis cartilage explants.
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Novel selective MMP-13 inhibitors reduce collagen degradation in bovine articular and human osteoarthritis cartilage explants.

机译:新型选择性MMP-13抑制剂降低了牛关节和人骨关节炎软骨外植物中的胶原降解。

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OBJECTIVE: MMP-13 is highly upregulated in arthritis and therefore strongly implicated in the pathogenesis of osteoarthritis (OA). Selective inhibition of MMP-13 may provide the desired cartilage degradation protection, while overcoming the musculoskeletal toxicity seen with nonselective inhibition of MMPs. METHODS: Activity and selectivity of novel MMP-13 inhibitors were determined in enzymatic and collagenase assays. Inhibition kinetics and competitive binding experiments were performed. The inhibition of collagen degradation was studied in cartilage explants from OA patients and in bovine and human articular cartilage systems. RESULTS: We have identified a new class of very potent and highly selective non-zinc-binding MMP-13 inhibitors. Selective MMP-13 inhibitors completely blocked type II collagen degradation in bovine explants and showed up to 80% inhibition in human OA cartilage. CONCLUSIONS: These results indicate MMP-13 as the primary collagenase in the human OA cartilage and in the IL-1/OSM-induced cartilage degradation process and suggest that selective MMP-13 inhibitors may be a potential treatment of OA.
机译:目的:MMP-13在关节炎中高度上调,因此在骨关节炎(OA)的发病机制中强烈意义。选择性抑制MMP-13可以提供所需的软骨降解保护,同时克服了对MMP的非选择性抑制的肌肉骨骼毒性。方法:在酶促和胶原酶测定中测定新型MMP-13抑制剂的活性和选择性。进行抑制动力学和竞争性结合实验。在来自OA患者和牛和人关节软骨系统的软骨外植体中研究了对胶原降解的抑制作用。结果:我们已经确定了一种新的非常有效和高选择性的非锌结合MMP-13抑制剂。选择性MMP-13抑制剂完全阻止II型胶原蛋白降解牛外植体,并在人类OA软骨中显示出高达80%的抑制。结论:这些结果表明MMP-13作为人OA软骨中的主要胶原酶和IL-1 / OSM诱导的软骨降解过程,并表明选择性MMP-13抑制剂可能是OA的潜在处理。

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