肺结节病模型中对弧菌蛋白和肉芽肿形成的全身免疫反应

IF 4.7 Q2 IMMUNOLOGY
Harini Bagavant , Katarzyna Cizio , Antonina M. Araszkiewicz , Joanna A. Papinska , Lori Garman , Chuang Li , Nathan Pezant , Wonder P. Drake , Courtney G. Montgomery , Umesh S. Deshmukh
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引用次数: 8

摘要

结节病的一个特征是对持续刺激的免疫反应失调,通常导致各器官形成非坏死性肉芽肿。虽然遗传易感性是疾病发展的重要因素,但结节病的病因尚不完全清楚。具体而言,自身免疫是否有助于疾病的发生或进展尚不确定。在这项研究中,我们研究了结节病患者对弧菌蛋白的全身自身免疫。检测了结节病患者和健康对照血清中人源蛋白IgG抗体。用重组小鼠弧菌蛋白免疫小鼠,静脉注射弧菌蛋白包被微球模拟肺结节病。研究了处理后小鼠肺的细胞浸润、肉芽肿形成和基因表达。用流式细胞术检测支气管肺泡灌洗液中的免疫细胞。与健康对照相比,结节病患者有更高的频率和循环抗vimentin IgG水平。静脉注射涂有弧菌素的微球后,免疫弧菌素的小鼠出现肺肉芽肿。这些结节样肉芽肿表现为朗汉斯和异物多核巨细胞、CD4 T细胞以及MHC II阳性和表达精氨酸酶1的巨噬细胞的异质集合。肺显示促炎基因表达上调,包括Ifng、Il17和Tnfa,反映结节病典型的TH1/TH17反应。此外,TH2典型通路的基因也上调,与支气管肺泡灌洗液中ILC2数量增加一致。总之,这些结果进一步证实了vimentin在结节病中的自身抗原作用,并为疾病发病机制中的抗vimentin免疫反应提供了证据。我们的研究还强调了ilc2驱动的th2样反应在结节病肺肉芽肿形成中的可能作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Systemic immune response to vimentin and granuloma formation in a model of pulmonary sarcoidosis

A characteristic feature of sarcoidosis is a dysregulated immune response to persistent stimuli, often leading to the formation of non-necrotizing granulomas in various organs. Although genetic susceptibility is an essential factor in disease development, the etiology of sarcoidosis is not fully understood. Specifically, whether autoimmunity contributes to the initiation or progression of the disease is uncertain. In this study, we investigated systemic autoimmunity to vimentin in sarcoidosis. IgG antibodies to human vimentin were measured in sera from sarcoidosis patients and healthy controls. Mice immunized with recombinant murine vimentin were challenged intravenously with vimentin-coated beads to mimic pulmonary sarcoidosis. Lungs from treated mice were studied for cellular infiltration, granuloma formation, and gene expression. Immune cells in the bronchoalveolar lavage fluid were evaluated by flow cytometry. Compared to healthy controls, sarcoidosis patients had a higher frequency and levels of circulating anti-vimentin IgG. Vimentin-immunized mice developed lung granulomas following intravenous challenge with vimentin-coated beads. These sarcoidosis-like granulomas showed the presence of Langhans and foreign body multinucleated giant cells, CD4 T cells, and a heterogeneous collection of MHC II positive and arginase 1-expressing macrophages. The lungs showed upregulated pro-inflammatory gene expression, including Ifng, Il17, and Tnfa, reflecting TH1/TH17 responses typical of sarcoidosis. In addition, genes in the TH2 canonical pathway were also upregulated, congruent with increased numbers of ILC2 in the bronchoalveolar lavage. Overall, these results further validate vimentin as an autoantigen in sarcoidosis and provide evidence for an anti-vimentin immune response in disease pathogenesis. Our study also highlights the possible role of ILC2-driven TH2-like responses in the formation of lung granulomas in sarcoidosis.

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来源期刊
Journal of Translational Autoimmunity
Journal of Translational Autoimmunity Medicine-Immunology and Allergy
CiteScore
7.80
自引率
2.60%
发文量
33
审稿时长
55 days
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