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先前接触邻苯二甲醛会增强二癸基二甲基氯化铵介导的 IgE 介导的免疫反应:两种常用抗菌剂协同增强过敏性疾病的潜力。

Prior Exposure to Ortho-Phthalaldehyde Augments IgE-Mediated Immune Responses to Didecyldimethylammonium Chloride: Potential for 2 Commonly Used Antimicrobials to Synergistically Enhance Allergic Disease.

机构信息

Allergy and Clinical Immunology Branch, Health Effects Laboratory Division, National Institute for Occupational Safety and Health, Morgantown, West Virginia 26505.

出版信息

Toxicol Sci. 2020 Nov 1;178(1):127-137. doi: 10.1093/toxsci/kfaa112.

Abstract

Health-care workers have an increased incidence of allergic disease compared with the general public and are exposed to a variety of high-level disinfectants. Although exposure to these agents has been associated with allergic disease, findings between epidemiology and animal studies often conflict respecting immunological mechanisms. Therefore, we hypothesized that previous exposure to a representative IgE-mediated sensitizer (ortho-phthalaldehyde [OPA]) alters immune responses to a representative T-cell-mediated sensitizer (didecyldimethlyammonium chloride [DDAC]). Here, BALB/c mice were topically exposed to OPA (0.5%) for 3 days, rested, then topically exposed to DDAC (0.0625%, 0.125%, and 0.25%) for 14 days. Coexposure resulted in phenotypic changes in draining lymph node (dLN) cells, including a decreased frequency of CD8+ T cells and increased frequency and number of B cells compared with DDAC-only treated mice. The coexposed mice also had enhanced Th2 responses, including significant alterations in: dLN Il4 (increased), B-cell activation (increased), CD8+ T-cell activation (decreased), and local and systemic IgE production (increased). These changes were not observed if mice were exposed to DDAC prior to OPA. Exposure to OPA alone shows Th2 skewing, indicated by increased activation of skin type 2 innate lymphoid cells, increased frequency and activation of draining lymph node B cells, and increased levels of type 2 cytokines. These findings suggest that the OPA-induced immune environment may alter the response to DDAC, resulting in increased IgE-mediated immune responses. This data may partially explain the discordance between epidemiological and laboratory studies regarding disinfectants and provide insight into the potential immunological implications of mixed chemical exposures.

摘要

医护人员比普通公众更容易患过敏性疾病,并且接触各种高水平消毒剂。尽管接触这些物质与过敏性疾病有关,但流行病学和动物研究的结果在免疫机制方面经常存在冲突。因此,我们假设先前接触代表性 IgE 介导的敏化剂(邻苯二醛[OPA])会改变对代表性 T 细胞介导的敏化剂(双癸基二甲基氯化铵[DDAC])的免疫反应。在这里,BALB/c 小鼠经皮暴露于 OPA(0.5%)3 天,休息后,然后经皮暴露于 DDAC(0.0625%、0.125%和 0.25%)14 天。共暴露导致引流淋巴结(dLN)细胞表型发生变化,包括与仅用 DDAC 处理的小鼠相比,CD8+T 细胞的频率降低,B 细胞的频率和数量增加。共暴露的小鼠还具有增强的 Th2 反应,包括:dLN Il4(增加)、B 细胞活化(增加)、CD8+T 细胞活化(减少)以及局部和全身 IgE 产生(增加)。如果小鼠在暴露于 OPA 之前先暴露于 DDAC,则不会观察到这些变化。单独暴露于 OPA 会导致 Th2 偏向,表现为皮肤 2 型固有淋巴细胞的活化增加、引流淋巴结 B 细胞的频率和活化增加以及 2 型细胞因子水平增加。这些发现表明,OPA 诱导的免疫环境可能改变对 DDAC 的反应,导致 IgE 介导的免疫反应增加。这些数据部分解释了流行病学和实验室研究在消毒剂方面的不一致,并为混合化学暴露的潜在免疫学意义提供了深入了解。

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Novel cutaneous mediators of chemical allergy.新型化学过敏皮肤介质。
J Immunotoxicol. 2019 Dec;16(1):13-27. doi: 10.1080/1547691X.2018.1515279. Epub 2019 Mar 1.

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