The role of interleukin 17 in the pathogenesis of rheumatoid arthritis. Are there any prospects for the use of IL-17 inhibitors?

E. Nasonov, A. Avdeeva, T. Korotaeva, T. Dubinina, J. V. Usacheva
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引用次数: 1

Abstract

Rheumatoid arthritis (RA) is an immunoinflammatory rheumatic disease (IMRI) characterized by chronic erosive arthritis and systemic damage to internal organs, leading to early disability and reduced life expectancy in patients. Thanks to the progress in the study of the mechanisms of the development of the IVRI and industrial biotechnology, new anti-inflammatory drugs have been created, the use of which has significantly increased the effectiveness of the pharmacotherapy of RA. However, the possibilities of pharmacotherapy for RA are limited, since all genetically engineered biological drugs (GEBDs), regardless of the mechanism of action, have approximately the same effectiveness in achieving remission. It is believed that the relatively unsatisfactory results of RA therapy are due to the heterogeneity of the mechanisms of inflammation. and pain. The significance of the Th17 type of immune response in the pathogenesis of RA, the results of controlled studies of IL-17 inhibitors, and the advisability of further studying the effectiveness of these drugs in patients with certain RA phenotypes are discussed.
白细胞介素17在类风湿关节炎发病机制中的作用。IL-17抑制剂的应用前景如何?
类风湿性关节炎(RA)是一种免疫炎症性风湿性疾病(IMRI),其特征是慢性糜糜性关节炎和内脏系统损伤,导致患者早期残疾和预期寿命缩短。由于IVRI发展机制的研究和工业生物技术的进步,新的抗炎药物被创造出来,其使用显著提高了RA药物治疗的有效性。然而,药物治疗RA的可能性是有限的,因为所有基因工程生物药物(gebd),无论其作用机制如何,在实现缓解方面都具有大致相同的有效性。人们认为,RA治疗的相对不理想的结果是由于炎症机制的异质性。和痛苦。本文讨论了Th17型免疫应答在RA发病机制中的意义,IL-17抑制剂的对照研究结果,以及进一步研究这些药物对某些RA表型患者的有效性的可行性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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