TCDD 和 CH223191 可改变 T 细胞平衡,但不能诱导成年狼疮小鼠的抗炎反应。

Q3 Medicine ImmunoHorizons Pub Date : 2024-02-01 DOI:10.4049/immunohorizons.2300023
Fernando Gutierrez, Quiyana M Murphy, Brianna K Swartwout, Kaitlin A Read, Michael R Edwards, Leila Abdelhamid, Xavier Cabana-Puig, James C Testerman, Tian Xu, Ran Lu, Pavly Amin, Thomas E Cecere, Christopher M Reilly, Kenneth J Oestreich, Stanca M Ciupe, Xin M Luo
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引用次数: 0

摘要

芳基烃受体(AhR)作为细胞膜受体、转录因子和 E3 泛素连接酶对内源性和外源性配体做出反应。一些研究支持 AhR 激活具有抗炎作用。然而,在发育早期暴露于 AhR 激动剂 2,3,7,8-四氯二苯并对二恶英(TCDD)会导致自身免疫表型并加重狼疮。TCDD对已存在自身免疫的成人狼疮的影响尚未被描述。我们利用一个成年小鼠模型提出了新的证据,证明TCDD刺激AhR会改变T细胞反应,但却不会影响狼疮样疾病。有趣的是,AhR 拮抗剂 CH223191 也改变了我们模型中的 T 细胞平衡。接下来,我们建立了一个概念框架,以确定导致狼疮生理结果的细胞和分子因素,并创建了描述细胞因子动态的模型,将其输入微分方程系统,以预测T滤泡辅助细胞(Tfh)和调节性T细胞(Treg)群的动力学。该模型预测,与车辆和 CH223191 相比,TCDD 暴露后 Tfh 细胞的扩增值更大。在最初升高之后,Tfh 和 Treg 细胞群随着时间的推移不断减少。基于预测的 Treg/Tfh 细胞比率的函数显示,在所有组中,Treg 细胞都超过了 Tfh 细胞,TCDD 和 CH223191 的 Treg/Tfh 细胞比率低于车辆,而且该比率随着时间的推移相对恒定。我们的结论是,AhR 配体不能诱导抗炎反应,从而减轻成年狼疮小鼠的自身免疫。这项研究对 TCDD 支持免疫抑制表型的教条提出了质疑。
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TCDD and CH223191 Alter T Cell Balance but Fail to Induce Anti-Inflammatory Response in Adult Lupus Mice.

Aryl hydrocarbon receptor (AhR) responds to endogenous and exogenous ligands as a cytosolic receptor, transcription factor, and E3 ubiquitin ligase. Several studies support an anti-inflammatory effect of AhR activation. However, exposure to the AhR agonist 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) during early stages of development results in an autoimmune phenotype and exacerbates lupus. The effects of TCDD on lupus in adults with pre-existing autoimmunity have not been described. We present novel evidence that AhR stimulation by TCDD alters T cell responses but fails to impact lupus-like disease using an adult mouse model. Interestingly, AhR antagonist CH223191 also changed T cell balance in our model. We next developed a conceptual framework for identifying cellular and molecular factors that contribute to physiological outcomes in lupus and created models that describe cytokine dynamics that were fed into a system of differential equations to predict the kinetics of T follicular helper (Tfh) and regulatory T (Treg) cell populations. The model predicted that Tfh cells expanded to larger values following TCDD exposure compared with vehicle and CH223191. Following the initial elevation, both Tfh and Treg cell populations continuously decayed over time. A function based on the ratio of predicted Treg/Tfh cells showed that Treg cells exceed Tfh cells in all groups, with TCDD and CH223191 showing lower Treg/Tfh cell ratios than the vehicle and that the ratio is relatively constant over time. We conclude that AhR ligands did not induce an anti-inflammatory response to attenuate autoimmunity in adult lupus mice. This study challenges the dogma that TCDD supports an immunosuppressive phenotype.

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