EGF-Receptor against Amphiregulin (AREG) Influences Costimulatory Molecules on Monocytes and T Cells and Modulates T-Cell Responses.

IF 3.5 3区 医学 Q2 IMMUNOLOGY Journal of Immunology Research Pub Date : 2023-11-24 eCollection Date: 2023-01-01 DOI:10.1155/2023/8883045
Stephan Dreschers, Christopher Platen, Louise Oppermann, Caitlin Doughty, Andreas Ludwig, Aaron Babendreyer, Thorsten W Orlikowsky
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Abstract

Amphiregulin (AREG) is a ligand of the epidermal growth factor receptor (EGFR) and has been shown to regulate the phagocytosis-induced cell death of monocytes in peripheral blood. AREG-dependent apoptotic signaling engages factors of the intrinsic and extrinsic apoptotic pathway, such as BCL-2, BCL-XL, and death ligand/receptor CD95/CD95L. Here, we tested the hypothesis that AREG influences costimulatory monocyte functions, which are crucial for T-cell responses. We found a stronger expression of AREG and EGFR in monocytes compared to lymphocytes. As a novel function of AREG, we observed reduced T-cell proliferation following polyclonal T-cell stimulation with OKT3. This reduction of proliferation occurred in the presence of monocytes as well as in their absence, monocyte signaling being replaced by crosslinking of OKT3. Increasing concentrations of AREG down-modulated the concentration of costimulatory B7 molecules (CD80/CD86) and HLA-DR on monocytes. In proliferation assays, CD28 expression on T cells was down-modulated on the application of OKT3 but unaltered by AREG. LcK activation, following OKT3-stimulation, was reduced in T cells that had been coincubated with AREG. The effects of AREG on T-cell phenotypes were also present when monocytes were depleted and OKT3 was crosslinked. The rearranged expression of immunological synapse proteins was accompanied by an alteration of T-cell polarization. Although the proportion of regulatory T cells was not shifted by AREG, IL-17-expressing T cells were significantly enhanced, with a bias toward TH1-polarization. Taken together, these results suggest that AREG acts as an immunoregulatory molecule at the interface between antigen-presenting cells and T cells.

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抗双调节蛋白egf受体(AREG)影响单核细胞和T细胞的共刺激分子并调节T细胞反应。
双调节蛋白(AREG)是表皮生长因子受体(EGFR)的一种配体,已被证明可调节吞噬诱导的外周血单核细胞死亡。areg依赖性凋亡信号通路涉及内源性和外源性凋亡通路的因子,如BCL-2、BCL-XL和死亡配体/受体CD95/CD95L。在这里,我们测试了AREG影响共刺激单核细胞功能的假设,这对t细胞反应至关重要。我们发现单核细胞中AREG和EGFR的表达强于淋巴细胞。作为AREG的新功能,我们观察到OKT3刺激多克隆t细胞后t细胞增殖减少。这种增殖的减少发生在单核细胞存在和不存在的情况下,单核细胞信号被OKT3交联所取代。增加AREG浓度可下调单核细胞上共刺激B7分子(CD80/CD86)和HLA-DR的浓度。在增殖实验中,使用OKT3可以下调T细胞上CD28的表达,而AREG则没有改变。在与AREG共孵育的T细胞中,okt3刺激后的LcK激活减少。当单核细胞耗尽和OKT3交联时,AREG对t细胞表型的影响也存在。免疫突触蛋白的重排表达伴随着t细胞极化的改变。虽然调节性T细胞的比例没有被AREG改变,但il -17表达的T细胞明显增强,并倾向于th1极化。综上所述,这些结果表明AREG在抗原呈递细胞和T细胞之间的界面上作为一种免疫调节分子。
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来源期刊
CiteScore
6.90
自引率
2.40%
发文量
423
审稿时长
15 weeks
期刊介绍: Journal of Immunology Research is a peer-reviewed, Open Access journal that provides a platform for scientists and clinicians working in different areas of immunology and therapy. The journal publishes research articles, review articles, as well as clinical studies related to classical immunology, molecular immunology, clinical immunology, cancer immunology, transplantation immunology, immune pathology, immunodeficiency, autoimmune diseases, immune disorders, and immunotherapy.
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