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新型细胞因子 IL27p28/IL12p40 通过抑制自身反应性 Th1/Th17 细胞和促进调节性 T 细胞的扩增来抑制实验性自身免疫性葡萄膜炎。

Novel IL27p28/IL12p40 cytokine suppressed experimental autoimmune uveitis by inhibiting autoreactive Th1/Th17 cells and promoting expansion of regulatory T cells.

机构信息

Molecular Immunology Section, Laboratory of Immunology, NEI, National Institutes of Health, Bethesda, Maryland 20892-1857, USA.

出版信息

J Biol Chem. 2012 Oct 19;287(43):36012-21. doi: 10.1074/jbc.M112.390625. Epub 2012 Aug 30.

Abstract

IL-12 family cytokines are important in host immunity. Whereas some members (IL-12, IL-23) play crucial roles in pathogenesis of organ-specific autoimmune diseases by inducing the differentiation of Th1 and Th17 lymphocytes, others (IL-27 and IL-35) suppress inflammatory responses and limit tissue injury induced by these T cell subsets. In this study, we have genetically engineered a novel IL27p28/IL12p40 heterodimeric cytokine (p28/p40) that antagonizes signaling downstream of the gp130 receptor. We investigated whether p28/p40 can be used to ameliorate uveitis, a CNS inflammatory disease. Experimental autoimmune uveitis (EAU) is the mouse model of human uveitis and is mediated by Th1 and Th17 cells. We show here that p28/p40 suppressed EAU by inhibiting the differentiation and inflammatory responses of Th1 and Th17 cells while promoting expansion of IL-10(+)- and Foxp3(+)-expressing regulatory T cells. Lymph node cells from mice treated with p28/p40 blocked adoptive transfer of EAU to naïve syngeneic mice by immunopathogenic T cells and suppressive effects of p28/p40 derived in part from antagonizing STAT1 and STAT3 pathways induced by IL-27 and IL-6. Interestingly, IL27p28 also suppressed EAU, but to a lesser extent than p28/p40. The inhibition of uveitogenic lymphocyte proliferation and suppression of EAU by p28/p40 and IL27p28 establish efficacy of single chain and heterodimeric IL-12 family cytokines in treatment of a CNS autoimmune disease. Creation of the biologically active p28/p40 heterodimeric cytokine represents an important proof-of-concept experiment, suggesting that cytokines comprising unique IL-12 α- and β-subunit pairing may exist in nature and may constitute a new class of therapeutic cytokines.

摘要

IL-12 家族细胞因子在宿主免疫中具有重要作用。虽然某些成员(IL-12、IL-23)通过诱导 Th1 和 Th17 淋巴细胞的分化在器官特异性自身免疫疾病的发病机制中发挥关键作用,但其他成员(IL-27 和 IL-35)则抑制炎症反应并限制这些 T 细胞亚群引起的组织损伤。在这项研究中,我们通过基因工程构建了一种新型的 IL27p28/IL12p40 异二聚体细胞因子(p28/p40),该因子拮抗 gp130 受体下游的信号转导。我们研究了 p28/p40 是否可用于改善葡萄膜炎,这是一种中枢神经系统炎症性疾病。实验性自身免疫性葡萄膜炎(EAU)是人类葡萄膜炎的小鼠模型,由 Th1 和 Th17 细胞介导。我们在此表明,p28/p40 通过抑制 Th1 和 Th17 细胞的分化和炎症反应,同时促进表达 IL-10(+)和 Foxp3(+)的调节性 T 细胞的扩增,从而抑制 EAU。用 p28/p40 处理的小鼠的淋巴结细胞通过免疫致病性 T 细胞阻断了 EAU 向同种异体 naive 小鼠的过继转移,并且 p28/p40 的抑制作用部分来自于拮抗由 IL-27 和 IL-6 诱导的 STAT1 和 STAT3 途径。有趣的是,IL27p28 也抑制了 EAU,但抑制程度低于 p28/p40。p28/p40 和 IL27p28 抑制致葡萄膜炎性淋巴细胞增殖和抑制 EAU 的作用,确立了单链和异二聚体 IL-12 家族细胞因子在治疗中枢神经系统自身免疫性疾病中的疗效。生物活性 p28/p40 异二聚体细胞因子的创建代表了一个重要的概念验证实验,表明包含独特的 IL-12 α-和 β-亚基配对的细胞因子可能存在于自然界中,并可能构成一类新的治疗性细胞因子。

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