The aryl hydrocarbon receptor differentially modulates the expression profile of antibody isotypes in a human B-cell line.

IF 3.4 3区医学 Q2 TOXICOLOGY Toxicological Sciences Pub Date : 2024-05-28 DOI:10.1093/toxsci/kfae035

Mili S Bhakta-Yadav, Kaulini Burra, Nasser Alhamdan, Clayton P Allex-Buckner, Courtney E W Sulentic

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Abstract

2,3,7,8-Tetrachlorodibenzo-p-dioxin (TCDD) is a persistent environmental contaminant and high affinity ligand for the aryl hydrocarbon receptor (AhR). In animal models, AhR activation by TCDD generally inhibits antibody secretion. However, it is less clear if this translates to human antibody production. Using a human Burkitt lymphoma B-cell line (CL-01) that can be stimulated to secrete Ig and undergo class switch recombination to other Ig isotypes, the current study evaluated the effects of AhR activation or antagonism on the human Ig isotypic expression profile with CD40L+IL-4 stimulation. Our results suggest that AhR agonists (TCDD and indirubin) have little to no effect on IgM or IgA secretion, which were also not induced with stimulation. However, AhR activation significantly inhibited stimulation-induced IgG secretion, an effect reversed by the AhR antagonist CH223191. Evaluation of Ig heavy chain (IgH) constant region gene expression (ie Cμ, Cγ1-4, Cα1-2, and Cε that encode for IgM, IgG1-4, IgA1-2, and IgE, respectively) demonstrated differential effects. While Cμ and Cα2 transcripts were unaffected by stimulation or AhR agonists, AhR activation significantly inhibited stimulation-induced Cγ2-4 and Cε mRNA transcripts, which was reversed by AhR antagonism. Notably, AhR antagonism in the absence of exogenous AhR ligands significantly increased IgG and IgA secretion as well as the expression of Cγ2-4 and Cε. These results suggest that modulation of AhR activity differentially alters the IgH isotypic expression profile and antibody secretion that may be partly dependent on cellular stimulation. Since a variety of chemicals from anthropogenic, industrial, pharmaceutical, dietary, and bacterial sources bind the AhR, the ability of environmental exposures to alter AhR activity (i.e. activate or inhibit) may have a direct influence on immune function and antibody-relevant disease conditions.

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芳基烃受体可对人类 B 细胞系中抗体同型的表达谱进行不同程度的调节。

2,3,7,8-四氯二苯并对二恶英（TCDD）是一种持久性环境污染物，也是芳基烃受体（AhR）的高亲和力配体。在动物模型中，TCDD 激活 AhR 通常会抑制抗体分泌。但是，这种情况是否会转化为人类抗体的产生还不太清楚。目前的研究使用了一种人类伯基特淋巴瘤 B 细胞系（CL-01），该细胞系可在 CD40L+IL-4 刺激下分泌 Ig 并进行类间转换重组为其他 Ig 同型，本研究评估了 AhR 激活或拮抗对人类 Ig 同型表达谱的影响。我们的结果表明，AhR 激动剂（TCDD 和靛玉红）对 IgM 或 IgA 的分泌几乎没有影响，刺激也不会诱导 IgM 或 IgA 的分泌。然而，AhR 激活会明显抑制刺激诱导的 IgG 分泌，AhR 拮抗剂 CH223191 可逆转这种效应。对 Ig 重链（IgH）恒定区基因表达（即分别编码 IgM、IgG1-4、IgA1-2 和 IgE 的 Cμ、Cγ1-4、Cα1-2 和 Cε）的评估显示了不同的效应。虽然 Cμ 和 Cα2 的转录不受刺激或 AhR 激动剂的影响，但 AhR 激活会显著抑制刺激诱导的 Cγ2-4 和 Cε mRNA 的转录，而 AhR 拮抗会逆转这种情况。值得注意的是，在没有外源 AhR 配体的情况下，AhR 拮抗可明显增加 IgG 和 IgA 的分泌以及 Cγ2-4 和 Cε 的表达。这些结果表明，对 AhR 活性的调节可不同程度地改变 IgH 同型表达谱和抗体分泌，而抗体分泌可能部分依赖于细胞刺激。由于来自人为、工业、医药、饮食和细菌的各种化学物质都与 AhR 结合，环境暴露改变 AhR 活性（即激活或抑制）的能力可能会直接影响免疫功能和抗体相关疾病。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Toxicological Sciences 医学-毒理学

CiteScore

7.70

自引率

7.90%

发文量

118

审稿时长

1.5 months

期刊介绍： The mission of Toxicological Sciences, the official journal of the Society of Toxicology, is to publish a broad spectrum of impactful research in the field of toxicology. The primary focus of Toxicological Sciences is on original research articles. The journal also provides expert insight via contemporary and systematic reviews, as well as forum articles and editorial content that addresses important topics in the field. The scope of Toxicological Sciences is focused on a broad spectrum of impactful toxicological research that will advance the multidisciplinary field of toxicology ranging from basic research to model development and application, and decision making. Submissions will include diverse technologies and approaches including, but not limited to: bioinformatics and computational biology, biochemistry, exposure science, histopathology, mass spectrometry, molecular biology, population-based sciences, tissue and cell-based systems, and whole-animal studies. Integrative approaches that combine realistic exposure scenarios with impactful analyses that move the field forward are encouraged.