Katia Mangano, Jose' Francisco Munoz-Valle, Claudia Azucena Palafox-Sánchez, Maria Cristina Petralia, Gian Marco Leone, Paolo Fagone, Ferdinando Nicoletti
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引用次数: 0
Abstract
This study aimed to investigate the role of TSPAN32, a member of the tetraspanin family, in rheumatoid arthritis (RA). The objective was to assess the expression levels of TSPAN32 in experimental RA models and in RA patient immune cells, exploring its potential as a regulatory factor in RA pathogenesis. The study employed adjuvant-induced arthritis in rats and collagen-induced arthritis (CIA) in mice as experimental models. Ex vivo analyses included evaluating TSPAN32 expression in immune cells at different stages of the disease. In silico data analysis involved examining transcriptomic datasets from drug-naïve and treated RA patients to correlate TSPAN32 expression with clinical parameters. TSPAN32 overexpression experiments in splenocytes from CIA mice aimed to demonstrate its functional impact on antigen-specific immune responses. The animal models revealed a significant downregulation of TSPAN32, particularly in synovial-infiltrating T cells. Also, TSPAN32 overexpression inhibited pro-inflammatory cytokine production in splenocytes. In RA patients, TSPAN32 was consistently downregulated in circulating and synovial-infiltrating T cells, as well as in CD8+ T cells, B cells and NK cells. Drug treatment did not significantly alter TSPAN32 levels. Negative correlations were observed between TSPAN32 expression and inflammatory markers (CRP, ESR) and clinical scores (SDAI) in RA patients. This study suggests that reduced TSPAN32 expression characterizes pathogenic T-cell populations in RA, highlighting its potential as biomarker for inflammation and disease activity. TSPAN32 may play a crucial role in shaping adaptive immune responses in RA, opening avenues for novel therapeutic strategies targeting this tetraspanin family member.
本研究旨在探讨四泛蛋白家族成员 TSPAN32 在类风湿性关节炎(RA)中的作用。目的是评估TSPAN32在实验性RA模型和RA患者免疫细胞中的表达水平,探索其作为RA发病机制调控因子的潜力。研究采用佐剂诱导的大鼠关节炎和胶原诱导的小鼠关节炎(CIA)作为实验模型。体内外分析包括评估疾病不同阶段免疫细胞中 TSPAN32 的表达。硅学数据分析包括检查未接受过药物治疗和接受过药物治疗的 RA 患者的转录组数据集,以将 TSPAN32 的表达与临床参数联系起来。TSPAN32在CIA小鼠脾细胞中的过表达实验旨在证明其对抗原特异性免疫反应的功能影响。动物模型显示 TSPAN32 的表达明显下调,尤其是在滑膜浸润 T 细胞中。此外,TSPAN32 的过表达抑制了脾细胞中促炎细胞因子的产生。在 RA 患者中,TSPAN32 在循环和滑膜浸润 T 细胞以及 CD8+ T 细胞、B 细胞和 NK 细胞中持续下调。药物治疗并未明显改变 TSPAN32 的水平。在 RA 患者中,TSPAN32 的表达与炎症指标(CRP、ESR)和临床评分(SDAI)之间呈负相关。这项研究表明,TSPAN32表达的减少是RA致病性T细胞群的特征,突出了其作为炎症和疾病活动生物标志物的潜力。TSPAN32可能在形成RA的适应性免疫反应中起着至关重要的作用,为针对这种四泛蛋白家族成员的新型治疗策略开辟了道路。
期刊介绍:
This peer-reviewed international journal publishes original articles and reviews on all aspects of basic, translational and clinical immunology. The journal aims to provide high quality service to authors, and high quality articles for readers.
The journal accepts for publication material from investigators all over the world, which makes a significant contribution to basic, translational and clinical immunology.