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首页> 外文期刊>Rheumatology international. >Evidence-based review of biologic markers as indicators of disease progression and remission in rheumatoid arthritis.
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Evidence-based review of biologic markers as indicators of disease progression and remission in rheumatoid arthritis.

机译:以生物标志物为基础的综述,作为类风湿关节炎疾病进展和缓解的指标。

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Rheumatoid arthritis (RA) is a chronic, immune-mediated inflammatory disease characterised by inflammation resulting in structural joint damage and functional disability. Tumour necrosis factor-alpha (TNFalpha) is a pivotal mediator and driver of inflammation in RA. Inflammation is closely related to the production of C-reactive protein (CRP), and a close correlation exists between serum CRP and TNFalpha levels. CRP levels are therefore a convenient, objective biomarker of disease activity. CRP correlates closely with changes in inflammation/disease activity, radiological damage and progression and functional disability. Identification of TNFalpha as a driver of RA progression has led to the introduction of TNFalpha-blocking agents and, subsequently, improvement of disease management. TNFalpha-blocking agents provide rapid, profound and sustained suppression of disease activity in correspondence with a marked reduction in CRP levels. A reduction in CRP level correlates closely with the positive clinical response to TNFalpha-blocking therapy. Thus, CRP levels can be used to predict, assess and monitor response to treatment with TNFalpha-blocking agents, and may be helpful in determining the optimal TNFalpha-blocker dosage. Given the close correlation between inflammation and disease progression and the relation between inflammation and CRP, the latter, if used effectively in clinical practice, may be means to identify patients likely to progress rapidly and who require intensive anti-TNFalpha therapy. The purpose of this review is to identify how CRP levels may be useful for monitoring the effect of therapy on halting disease progression and why monitoring CRP levels at baseline and after treatment should become a routine part of clinical practice.
机译:类风湿关节炎(RA)是一种慢性的,免疫介导的炎症性疾病,其特征在于炎症导致结构性关节损伤和功能障碍。肿瘤坏死因子-α(TNFalpha)是RA的关键介质和炎症驱动因子。炎症与C反应蛋白(CRP)的产生密切相关,并且血清CRP与TNFalpha水平之间存在密切相关。因此,CRP水平是疾病活动的便捷,客观的生物标记。 CRP与炎症/疾病活动,放射损伤,进展和功能障碍的变化密切相关。 TNFα作为RA进展的驱动因素的鉴定导致了TNFalpha阻断剂的引入,并因此改善了疾病的管理。 TNFα阻断剂可迅速,深刻和持续地抑制疾病活动,并显着降低CRP水平。 CRP水平的降低与对TNFalpha阻断疗法的积极临床反应密切相关。因此,CRP水平可用于预测,评估和监测对TNFα阻断剂治疗的反应,并且可能有助于确定最佳的TNFα阻断剂剂量。考虑到炎症和疾病进展之间的密切相关以及炎症和CRP之间的关系,如果CRP在临床实践中得到有效使用,则可能是鉴定可能快速进展且需要强化抗TNFα治疗的患者的手段。这篇综述的目的是确定CRP水平如何用于监测治疗对中止疾病进展的影响,以及为什么在基线和治疗后监测CRP水平应成为临床实践的常规内容。

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