在自身免疫性肠道炎症过程中,B细胞介导的CD4 T细胞通过CD86的共刺激加剧了促炎细胞因子的产生。

IF 7.9 2区 医学 Q1 IMMUNOLOGY
Iana Gadjalova , Julia M. Heinze , Marie C. Goess , Julian Hofmann , Annalisa Buck , Marie-Christin Weber , Birgit Blissenbach , Maximilian Kampick , Oleg Krut , Katja Steiger , Klaus-Peter Janssen , Philipp-Alexander Neumann , Jürgen Ruland , Selina J. Keppler
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引用次数: 0

摘要

炎症性肠病(IBD)患者的B细胞反应失调;然而,B细胞在IBD病理中的作用仍不完全清楚。我们在此为活化的B细胞在自身免疫性肠道炎症发作过程中的有害作用提供了证据。使用Wiskott-Aldrich综合征相互作用蛋白缺陷(Wipf1-/-)小鼠作为慢性结肠炎的小鼠模型,我们确定活化的B细胞上CD86的表达是加剧肠道CD4 T细胞促炎细胞因子产生的关键因素。在我们的慢性IBD小鼠模型中,通过抗CD20抗体治疗消耗B细胞或通过CTLA-4-Ig阻断CD86介导的共刺激信号可在疾病发作时减轻肠道炎症。这是由于异常体液免疫反应减少,CD4 T细胞促炎细胞因子产生减少,尤其是IFN-γ和GM-CSF。有趣的是,除了从Wipf1-/-小鼠炎症结肠中分离的B细胞外,我们还发现从人类IBD患者炎症组织中分离的活化B细胞上CD86mRNA和蛋白表达上调。我们在小鼠和人IBD患者的血清中发现,可溶性CD40L在体外促进了B细胞的活化和CD86的表达。总之,我们的数据为B细胞对肠道炎症的贡献提供了详细的见解,对IBD的治疗有启示。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
B cell-mediated CD4 T-cell costimulation via CD86 exacerbates pro-inflammatory cytokine production during autoimmune intestinal inflammation

Dysregulated B cell responses have been described in inflammatory bowel disease (IBD) patients; however, the role of B cells in IBD pathology remained incompletely understood. We here provide evidence for the detrimental role of activated B cells during the onset of autoimmune intestinal inflammation. Using Wiskott-Aldrich Syndrome interacting protein deficient (Wipf1−/−) mice as a mouse model of chronic colitis, we identified clusters of differentiation (CD)86 expression on activated B cells as a crucial factor exacerbating pro-inflammatory cytokine production of intestinal CD4 T cells. Depleting B cells through anti-CD20 antibody treatment or blocking costimulatory signals mediated by CD86 through cytotoxic T lymphocyte antigen-4-immunoglobulin (CTLA-4-Ig) diminished intestinal inflammation in our mouse model of chronic IBD at the onset of disease. This was due to a reduction in aberrant humoral immune responses and reduced CD4 T cell pro-inflammatory cytokine production, especially interferon-g (IFN-g) and granulocyte-macrophage colony-stimulating factor (GM-CSF). Interestingly, in addition to B cells isolated from the inflamed colon of Wipf1−/− mice, we also found CD86 mRNA and protein expression upregulated on activated B cells isolated from inflamed tissue of human patients with IBD. B cell activation and CD86 expression were boosted by soluble CD40L in vitro, which we found in the serum of mice and human patients with IBD. In summary, our data provides detailed insight into the contribution of B cells to intestinal inflammation, with implications for the treatment of IBD.

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来源期刊
Mucosal Immunology
Mucosal Immunology 医学-免疫学
CiteScore
16.60
自引率
3.80%
发文量
100
审稿时长
12 days
期刊介绍: Mucosal Immunology, the official publication of the Society of Mucosal Immunology (SMI), serves as a forum for both basic and clinical scientists to discuss immunity and inflammation involving mucosal tissues. It covers gastrointestinal, pulmonary, nasopharyngeal, oral, ocular, and genitourinary immunology through original research articles, scholarly reviews, commentaries, editorials, and letters. The journal gives equal consideration to basic, translational, and clinical studies and also serves as a primary communication channel for the SMI governing board and its members, featuring society news, meeting announcements, policy discussions, and job/training opportunities advertisements.
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