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首页> 外文期刊>Current Opinion in Molecular Therapeutics >An update on pharmacogenomics in rheumatoid arthritis with a focus on TNF-blocking agents.
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An update on pharmacogenomics in rheumatoid arthritis with a focus on TNF-blocking agents.

机译:类风湿关节炎药物基因组学的最新进展,重点是TNF阻断剂。

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TNFalpha is a proinflammatory cytokine, which is crucial in the pathogenesis of rheumatoid arthritis (RA). In recent years, biological therapies which block the damaging effects of TNFalpha on synovium and cartilage have been developed. TNF antagonists, such as etanercept, infliximab and adalimumab, although highly effective in RA, are expensive, totaling several thousand US dollars in yearly costs. In addition, only approximately 60% of patients respond to these agents. This has led to the need to prospectively identify patients most likely to respond to these agents, which can be achieved by pharmacogenomics approaches. Polymorphisms in genes encoding for TNFalpha, the MHC region, and the Fcgamma receptor IIIA, as well as their ability to predict disease progression in RA and response to anti-TNF therapies, have been the focus of a number of studies, which are discussed in this review. There is no consensus at present as to whether pharmacogenomics will allow prediction of anti-TNF therapy efficacy in RA. Large, prospective, multicenter studies are needed to replicate and validate the results of the studies outlined in this review.
机译:TNFalpha是一种促炎性细胞因子,在类风湿关节炎(RA)的发病机理中至关重要。近年来,已经开发了阻止TNFα对滑膜和软骨的破坏作用的生物疗法。 TNF拮抗剂,例如依那西普,英夫利昔单抗和阿达木单抗,尽管在RA中非常有效,但价格昂贵,每年的总成本为数千美元。此外,只有大约60%的患者对这些药物有反应。这导致需要前瞻性地确定最可能对这些药物产生反应的患者,这可以通过药物基因组学方法来实现。编码TNFalpha,MHC区和Fcgamma受体IIIA的基因的多态性,以及它们预测RA中疾病进展和对抗TNF治疗的反应的能力,已成为许多研究的重点,这些研究已在以下文献中讨论。这次审查。关于药物基因组学是否可以预测RA的抗TNF治疗功效,目前尚无共识。需要大型,前瞻性,多中心研究来复制和验证本综述中概述的研究结果。

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