Murine Skin Carcinogenesis and the Role of Immune System Dysregulation in the Tumorigenicity of 2-Ethylhexyl Acrylate.

Biomedicine Hub Pub Date : 2020-09-02 eCollection Date: 2020-05-01 DOI:10.1159/000508295
Craig A Elmets, Nabiha Yusuf
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引用次数: 3

Abstract

Some chemicals act as human carcinogens in various organ systems including the skin. Mice have been an ideal model to study a wide variety of chemical carcinogens because the pathogenesis in that species often mirrors that in humans. However, different mouse strains vary in their susceptibility to these agents. Thus, reliance on a single strain may lead to inaccurate findings. 2-Ethylhexyl acrylate (2-EHA) is an acrylate used as a co-monomer in the production of polymer resins for adhesives, latex paints, cross-linking agents, finishes for textiles and leather, and paper coatings. Monomer exposure may occur in occupational settings where it is produced or used; the only exposure that may occur to consumers or construction personnel is trace amounts in the final polymer product. There are no reports of cancer in humans caused by exposure to 2-EHA. However, 2-EHA has been reported to cause cancer in one strain of mice. This is an important issue since recommendations about its safety in humans depend, in part, on information derived from animal studies. We reviewed the literature on the preclinical effects of acrylates on skin carcinogenesis in C3H/HeJ mice, which can be criticized because of peculiarities in the immunological composition of that strain, the lack of rigorous histopathologic characterization of tumors that developed, the high doses of 2-EHA that were used for evaluation, and the lack of reproducibility in a second strain of mice. The C3H/HeJ mouse model is not ideal as it has a mutation in Toll-like receptor 4 (TLR4) that impairs its innate and adaptive immune responses. Inconsistencies in the histological evaluation of tumors induced in C3H/HeJ mice provide further evidence that the tumorigenic effect of 2-EHA was strain specific, a result of chronic inflammation during the promotion stage and/or a skewed immune response caused by the TLR4 mutation. In conclusion, 2-EHA has not convincingly been demonstrated to have skin carcinogenic activity to date. More relevant mouse models that mimic human squamous cell carcinoma, basal cell carcinoma, and melanoma with amounts that do not exceed a maximum tolerated dose are needed to assess the carcinogenic effects of 2-EHA.

小鼠皮肤癌变及免疫系统失调在2-乙基己基丙烯酸酯致瘤性中的作用。
一些化学物质在包括皮肤在内的各种器官系统中充当人类致癌物。小鼠一直是研究多种化学致癌物的理想模型,因为该物种的发病机制往往反映了人类的发病机制。然而,不同的小鼠品系对这些药物的易感性不同。因此,对单一菌株的依赖可能导致不准确的结果。2-乙基己基丙烯酸酯(2-EHA)是一种丙烯酸酯,用作共聚单体,用于生产粘合剂、乳胶漆、交联剂、纺织品和皮革涂饰以及纸张涂料的聚合物树脂。单体暴露可能发生在生产或使用单体的职业环境中;消费者或施工人员唯一可能接触到的是最终聚合物产品中的微量。目前还没有因暴露于2-EHA而导致人类癌症的报告。然而,据报道,2-EHA在一种小鼠中致癌。这是一个重要的问题,因为关于其在人类中的安全性的建议部分取决于来自动物研究的信息。我们回顾了关于丙烯酸酯对C3H/HeJ小鼠皮肤癌变的临床前作用的文献,这些文献可能受到批评,因为该菌株的免疫组成的特殊性,肿瘤发展缺乏严格的组织病理学特征,用于评估的高剂量2-EHA,以及在第二种小鼠中缺乏可重复性。C3H/HeJ小鼠模型并不理想,因为它在toll样受体4 (TLR4)中发生突变,损害其先天和适应性免疫反应。在C3H/HeJ小鼠中诱导的肿瘤组织学评价的不一致进一步证明了2-EHA的致瘤作用是菌株特异性的,是促进阶段慢性炎症和/或TLR4突变引起的扭曲免疫反应的结果。总之,到目前为止,2-EHA还没有令人信服的证明具有皮肤致癌活性。需要更多相关的小鼠模型来模拟人类鳞状细胞癌、基底细胞癌和黑色素瘤,其剂量不超过最大耐受剂量,以评估2-EHA的致癌作用。
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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