Association of M2 Macrophages, Th2, and B Cells With Pathomechanism in Microscopic Polyangiitis Complicated by Interstitial Lung Disease

S. Matsuda, T. Kotani, H. Kuwabara, Takayasu Suzuka, Takao Kiboshi, Y. Wada, T. Ishida, Youhei Fujiki, Hideyuki Shiba, K. Hata, T. Shoda, Y. Hirose, T. Takeuchi
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引用次数: 1

Abstract

Objective To address the pathomechanism of microscopic polyangiitis (MPA) complicated by interstitial lung disease (ILD) using serum biomarker profile and pulmonary histopathology. Methods Serum biomarkers from patients with MPA-ILD (n = 32), MPA without ILD (n = 17), and healthy controls (n = 10) were examined. Based on the biomarker profiles, principal component analysis (PCA) and cluster analysis were performed to classify patients with MPA-ILD into subgroups. Clinical characteristics and prognosis were assessed for each subgroup. Two lung biopsies were examined following H&E staining and immunostaining. Results T cell and macrophage polarization was skewed toward the T helper (Th) 2 cells and M2 macrophages in the MPA-ILD group relative to that in MPA without ILD group. The PCA allowed classification of the 19 biomarker profiles into 3 groups: (1) B cell– and neutrophil-related cytokines, vascular angiogenesis-related factors, extracellular matrix-producing factors; (2) Th1-driven cytokines, M1 macrophage-driven cytokines, and Th2-driven cytokines; and (3) M2 macrophage-induced and driven cytokines. The cluster analysis stratified the patients with MPA-ILD into clinically fibrotic-dominant (CFD) and clinically inflammatory-dominant (CID) groups. Notably, severe infections were significantly higher in the CFD group than in the CID group. Immunohistochemical staining demonstrated intense CXC motif chemokine ligand 13 staining in B cells and Th2 cells in the interstitium of the lungs of patients with MPA-ILD. Conclusion. The activation of M2 macrophages, Th2 cells, and B cells plays a key role in the pathomechanism of MPA-ILD. Classification of MPA-ILD based on serum biomarker profile would be useful in predicting the disease activity and the complications of severe infection in MPA-ILD.
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M2巨噬细胞、Th2和B细胞与显微多血管炎合并间质性肺疾病的病理机制的关联
目的探讨显微多血管炎(MPA)并发间质性肺疾病(ILD)的病理机制。方法对MPA-ILD患者(n = 32)、MPA无ILD患者(n = 17)和健康对照(n = 10)的血清生物标志物进行检测。基于生物标志物特征,采用主成分分析(PCA)和聚类分析对MPA-ILD患者进行亚组分类。评估每个亚组的临床特征和预后。2例肺活检行H&E染色和免疫染色。结果MPA-ILD组的T细胞和巨噬细胞极化倾向于辅助性T (Th) 2细胞和M2巨噬细胞。PCA允许将19个生物标志物分为3组:(1)B细胞和中性粒细胞相关细胞因子,血管生成相关因子,细胞外基质生成因子;(2) th1驱动型细胞因子、M1巨噬细胞驱动型细胞因子、th2驱动型细胞因子;(3) M2巨噬细胞诱导和驱动的细胞因子。聚类分析将MPA-ILD患者分为临床纤维化优势组(CFD)和临床炎症优势组(CID)。值得注意的是,CFD组的严重感染明显高于CID组。免疫组化染色显示MPA-ILD患者肺间质B细胞和Th2细胞中强烈的CXC基序趋化因子配体13染色。结论。M2巨噬细胞、Th2细胞和B细胞的活化在MPA-ILD的发病机制中起关键作用。基于血清生物标志物的MPA-ILD分类将有助于预测MPA-ILD的疾病活动性和严重感染的并发症。
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The Journal of rheumatology. Supplement
The Journal of rheumatology. Supplement Medicine-Medicine (all)
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期刊介绍: The Journal of Rheumatology is a monthly international serial edited by Duncan A. Gordon, The Journal features research articles on clinical subjects from scientists working in rheumatology and related fields, as well as proceedings of meetings as supplements to regular issues. Highlights of our 36 years serving Rheumatology include: groundbreaking and provocative editorials such as "Inverting the Pyramid," renowned Pediatric Rheumatology, proceedings of OMERACT and the Canadian Rheumatology Association, Cochrane Musculoskeletal Reviews, and supplements on emerging therapies.
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