通过Toll样受体驱动途径的反复局部激活诱导的慢性破坏性小鼠关节炎的T细胞依赖性：白细胞介素-1β和白细胞介素-17的关键作用

T cell dependence of chronic destructive murine arthritis induced by repeated local activation of Toll-like receptor-driven pathways: crucial role of both interleukin-1beta and interleukin-17.

作者信息

Joosten Leo A B, Abdollahi-Roodsaz Shahla, Heuvelmans-Jacobs Marleen, Helsen Monique M A, van den Bersselaar Liduine A M, Oppers-Walgreen Birgitte, Koenders Marije I, van den Berg Wim B

机构信息

Radboud University Nijmegen Medical Centre, Nijmegen, The Netherlands.

出版信息

Arthritis Rheum. 2008 Jan;58(1):98-108. doi: 10.1002/art.23152.

DOI:10.1002/art.23152

PMID:18163514

Abstract

OBJECTIVE

The pathogenesis of rheumatoid arthritis is often linked to bacterial infections. The present study was undertaken to develop a mouse model of chronic destructive arthritis induced by repeated intraarticular (IA) exposure to bacterial cell wall fragments and to investigate the cytokine dependence of this model.

METHODS

Mice that were deficient in various cytokines were injected IA with cell wall fragments of Streptococcus pyogenes on days 0, 7, 14, and 21. The development of chronic destructive arthritis was compared between groups of mice lacking different cytokines, to assess which cytokines were crucial for development of chronic destructive arthritis.

RESULTS

Repeated exposure of a joint to S pyogenes cell wall fragments resulted in the development of chronic destructive arthritis. In mice deficient in recombination-activating gene 2, streptococcal cell wall (SCW)-directed T cell reactivity was found and chronic arthritis did not develop, implicating T cells in the generation of chronic SCW-induced arthritis. Interleukin-17 (IL-17) receptor-deficient mice showed a reduction of joint destruction in the chronic stage, implicating a detrimental role of the recently discovered IL-17-producing T helper cells (Th17 cells). IL-23 expression was apparent during the late stages of arthritis. Joint swelling was no longer dependent on tumor necrosis factor alpha (TNFalpha) after the last flare, and pronounced cartilage damage was found after 28 days in TNFalpha-deficient mice. In contrast, IL-1beta-deficient mice were fully protected against joint swelling and cartilage and bone destruction during the late stages of disease.

CONCLUSION

These findings indicate that the TNFalpha dependence of arthritis is lost during the erosive stage, when Th17 cells become crucial. IL-1beta dependence remains strong, consistent with its pivotal role in the generation of Th17 cells.

摘要

目的

类风湿关节炎的发病机制常与细菌感染有关。本研究旨在建立一种通过反复关节内（IA）注射细菌细胞壁片段诱导的慢性破坏性关节炎小鼠模型，并研究该模型对细胞因子的依赖性。

方法

在第0、7、14和21天，对各种细胞因子缺陷的小鼠进行IA注射化脓性链球菌细胞壁片段。比较缺乏不同细胞因子的小鼠组慢性破坏性关节炎的发展情况，以评估哪些细胞因子对慢性破坏性关节炎的发展至关重要。

结果

关节反复暴露于化脓性链球菌细胞壁片段会导致慢性破坏性关节炎的发展。在重组激活基因2缺陷的小鼠中，发现了针对链球菌细胞壁（SCW）的T细胞反应性，且未发生慢性关节炎，这表明T细胞参与了慢性SCW诱导的关节炎的发生。白细胞介素-17（IL-17）受体缺陷的小鼠在慢性期关节破坏减少，这表明最近发现的产生IL-17的辅助性T细胞（Th17细胞）起了有害作用。IL-23表达在关节炎后期明显。在最后一次发作后，关节肿胀不再依赖肿瘤坏死因子α（TNFα），且在TNFα缺陷小鼠中，28天后发现明显的软骨损伤。相比之下，IL-1β缺陷小鼠在疾病后期完全免受关节肿胀以及软骨和骨破坏的影响。