ADAMTS-4 (aggrecanase1) is believed to play an important role in the degradation of aggrecan during the progression of joint diseases. ADAMTS-4 is synthesized as a latent pro-enzyme that requires the removal of the pro-domain, exposing the N-terminal neoepitope, to achieve activity. We developed a monoclonal antibody against this neoepitope of active ADAMTS-4. Furthermore, we established and characterized a competitive ELISA for measuring active ADAMTS-4 form applying the specific antibody. We used this assay to profile the presence of active ADAMTS-4 and its aggrecan degradation product (NITEGE(373)) in a bovine cartilage ex vivo model. We found that after stimulation with catabolic factors, the cartilage initially released high levels of aggrecanase-derived aggrecan fragments into supernatant but subsequently decreased to background levels. The level of active ADAMTS-4 released into the supernatant and retained in the cartilage matrix increased continuously throughout the 21days of the study. The activity of ADAMTS-4 on the last day of catabolic stimulation was verified in vitro by adding deglycosylated or native aggrecan to the conditioned medium. Samples of human cartilage affected by varying degrees of osteoarthritis stained strongly for active ADAMTS-4 where surface fibrillation and clustered chondrocytes were observed. This assay could be an effective tool for studying ADAMTS-4 activity and for screening drugs regulating ADAMTS-4 activation. Moreover, it could be a potential biomarker for degenerative joint disease.

译文

:ADAMTS-4(aggrecanase1)被认为在关节疾病进展期间在聚集蛋白聚糖的降解中起重要作用。 ADAMTS-4被合成为潜在的原酶,需要去除原结构域,暴露N末端新表位才能达到活性。我们开发了针对活性ADAMTS-4的这种新表位的单克隆抗体。此外,我们建立并鉴定了一种竞争性ELISA,用于测量应用特异性抗体的活性ADAMTS-4形式。我们使用此测定法分析了牛软骨离体模型中活性ADAMTS-4及其蛋白聚糖降解产物(NITEGE(373))的存在。我们发现,在分解代谢因子刺激后,软骨最初将高水平的软骨聚集蛋白聚糖酶衍生的软骨聚集蛋白片段释放到上清液中,但随后降至背景水平。在整个研究的21天中,释放到上清液中并保留在软骨基质中的活性ADAMTS-4的水平持续增加。通过在条件培养基中添加去糖基化的或天然的聚集蛋白聚糖,体外验证了分解代谢刺激的最后一天ADAMTS-4的活性。受不同程度的骨关节炎影响的人类软骨样品对活跃的ADAMTS-4进行了强烈染色,其中观察到了表面纤颤和聚集的软骨细胞。该测定法可能是研究ADAMTS-4活性和筛选调节ADAMTS-4活化的药物的有效工具。此外,它可能是退行性关节疾病的潜在生物标志物。

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