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免疫介导的炎症性关节炎中的白细胞介素-20受体轴:天然免疫识别与骨稳态之间的新联系。

The IL-20 receptor axis in immune-mediated inflammatory arthritis: novel links between innate immune recognition and bone homeostasis.

作者信息

Kragstrup T W

机构信息

a Department of Biomedicine , Aarhus University , Aarhus , Denmark.

b Department of Rheumatology , Aarhus University Hospital , Aarhus , Denmark.

出版信息

Scand J Rheumatol. 2016 Aug;45(sup128):53-57. doi: 10.1080/03009742.2016.1203022.

DOI:10.1080/03009742.2016.1203022
PMID:27687482
Abstract

The treatment of rheumatoid arthritis (RA) and spondyloarthritis (SpA) was transformed a little over a decade ago by the introduction of agents neutralizing the pro-inflammatory cytokine tumour necrosis factor (TNF)-α. Nevertheless, some patients do not achieve remission and the inhibition of the normal immune system with current drugs increases the risk of infection. The interleukin (IL)-20 receptor (IL-20R) axis is pivotal for tissue homeostasis. By contrast, this axis does not seem to directly activate cells of the immune system. Thus, modulation of the IL-20R axis might not result in increased risk of infection. The IL-20R axis consists of the three cytokines IL-19, IL-20, and IL-24 (termed the IL-20R cytokines) and their shared receptors. All three cytokines bind the receptor complex of IL-20R2/IL-20R1 whereas only IL-20 and IL-24 also bind the receptor complex of IL-20R2/IL-22R1. This short review describes how the IL-20R axis could be a novel link between innate immune recognition and bone homeostasis. The IL-20R cytokines are produced in response to both danger-associated molecular patterns and immune complexes formed by RA-associated autoantibodies. This could be of importance because these mediators can thus be present even in situations without inflammation. IL-19 shows anti-inflammatory properties in arthritis through IL-20R1. IL-20 and IL-24 through IL-22R seem to participate in the recruitment of mononuclear cells to the synovial joint and to sites of bone erosion in particular. Our results indicate that dual inhibition of IL-20 and IL-24 or attenuation of the shared IL-22R subunit could have a beneficial effect on radiographic progression, especially in seropositive RA.

摘要

十多年前,通过引入中和促炎细胞因子肿瘤坏死因子(TNF)-α的药物,类风湿性关节炎(RA)和脊柱关节炎(SpA)的治疗发生了变革。然而,一些患者并未实现缓解,并且当前药物对正常免疫系统的抑制增加了感染风险。白细胞介素(IL)-20受体(IL-20R)轴对于组织稳态至关重要。相比之下,该轴似乎不会直接激活免疫系统细胞。因此,调节IL-20R轴可能不会增加感染风险。IL-20R轴由三种细胞因子IL-19、IL-20和IL-24(称为IL-20R细胞因子)及其共享受体组成。所有这三种细胞因子都与IL-20R2/IL-20R1的受体复合物结合,而只有IL-20和IL-24也与IL-20R2/IL-22R1的受体复合物结合。这篇简短的综述描述了IL-20R轴如何可能成为先天免疫识别与骨稳态之间的新联系。IL-20R细胞因子是在对危险相关分子模式和由RA相关自身抗体形成的免疫复合物作出反应时产生的。这可能很重要,因为即使在没有炎症的情况下这些介质也可能存在。IL-19通过IL-20R1在关节炎中表现出抗炎特性。IL-20和IL-24通过IL-22R似乎尤其参与单核细胞向滑膜关节和骨侵蚀部位的募集。我们的结果表明,对IL-20和IL-24的双重抑制或对共享的IL-22R亚基的减弱可能对影像学进展有有益影响,尤其是在血清阳性RA中。

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