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硫柳汞对小鼠的免疫抑制和自身免疫作用。

Immunosuppressive and autoimmune effects of thimerosal in mice.

作者信息

Havarinasab S, Häggqvist B, Björn E, Pollard K M, Hultman P

机构信息

Department of Molecular and Clinical Medicine, Molecular and Immunological Pathology (AIR), Linköping University, SE-581 85 Linköping, Sweden.

出版信息

Toxicol Appl Pharmacol. 2005 Apr 15;204(2):109-21. doi: 10.1016/j.taap.2004.08.019.

Abstract

The possible health effects of the organic mercury compound thimerosal (ethylmercurithiosalicylate), which is rapidly metabolized to ethylmercury (EtHg), have recently been much debated and the effect of this compound on the immune system is largely unknown. We therefore studied the effect of thimerosal by treating A.SW (H-2s) mice, susceptible to induction of autoimmunity by heavy metals, with 10 mg thimerosal/L drinking water (internal dose ca 590 microg Hg/kg body weight/day) for up to 30 days. The lymph node expression of IL-2 and IL-15 mRNA was increased after 2 days, and of IL-4 and IFN-gamma mRNA after 6 and 14 days. During the first 14 days treatment, the number of splenocytes, including T and B cells as well as Ig-secreting cells decreased. A strong immunostimulation superseded after 30 days treatment with increase in splenic weight, number of splenocytes including T and B cells and Ig-secreting cells, and Th2- as well as Th-1-dependent serum immunoglobulins. Antinucleolar antibodies (ANoA) targeting the 34-kDa nucleolar protein fibrillarin, and systemic immune-complex deposits developed. The H-2s strains SJL and B10.S also responded to thimerosal treatment with ANoA. The A.TL and B10.TL strain, sharing background genes with the A.SW and B10.S strain, respectively, but with a different H-2 haplotype (t1), did not develop ANoA, linking the susceptibility to H-2. Thimerosal-treated H-2s mice homozygous for the nu mutation (SJL-nu/nu), or lacking the T-cell co-stimulatory molecule CD28 (B10.S-CD28-/-), did not develop ANoA, which showed that the autoimmune response is T-cell dependent. Using H-2s strains with targeted mutations, we found that IFN-gamma and IL-6, but not IL-4, is important for induction of ANoA by thimerosal. The maximum added renal concentration of thimerosal (EtHg) and inorganic mercury occurred after 14 days treatment and was 81 microg Hg/g. EtHg made up 59% and inorganic mercury 41% of the renal mercury. In conclusion, the organic mercury compound thimerosal (EtHg) has initial immunosuppressive effects similar to those of MeHg. However, in contrast to MeHg, thimerosal treatment leads in genetically susceptible mice to a second phase with strong immunostimulation and autoimmunity, which is T-cell dependent, H-2 linked and may at least partly be due to the inorganic mercury derived from the metabolism of ethyl mercury.

摘要

有机汞化合物硫柳汞(乙基汞硫代水杨酸盐)可迅速代谢为乙基汞(EtHg),其对健康可能产生的影响近来备受争议,而且该化合物对免疫系统的影响在很大程度上尚不清楚。因此,我们通过用含10mg硫柳汞/升饮用水(体内剂量约590μg汞/千克体重/天)处理易被重金属诱导自身免疫的A.SW(H-2s)小鼠,最长处理30天,来研究硫柳汞的作用。处理2天后,白细胞介素-2(IL-2)和白细胞介素-15(IL-15)mRNA的淋巴结表达增加,处理6天和14天后,IL-4和干扰素-γ(IFN-γ)mRNA的表达增加。在处理的前14天,脾细胞数量减少,包括T细胞、B细胞以及分泌免疫球蛋白的细胞。处理30天后,出现强烈的免疫刺激,脾脏重量增加,包括T细胞、B细胞以及分泌免疫球蛋白的细胞在内的脾细胞数量增加,Th2以及Th1依赖性血清免疫球蛋白增加。出现了靶向34kDa核仁蛋白纤维原蛋白的抗核仁抗体(ANoA)以及全身性免疫复合物沉积。H-2s品系SJL和B10.S对硫柳汞处理也产生了ANoA反应。分别与A.SW和B10.S品系共享背景基因,但具有不同H-2单倍型(t1)的A.TL和B10.TL品系未产生ANoA,这表明易感性与H-2有关。用nu突变纯合的硫柳汞处理的H-(2s)小鼠(SJL-nu/nu),或缺乏T细胞共刺激分子CD28的小鼠(B10.S-CD28-/-)未产生ANoA,这表明自身免疫反应是T细胞依赖性的。使用具有靶向突变的H-2s品系,我们发现IFN-γ和IL-6对硫柳汞诱导ANoA很重要,而IL-4则不然。处理14天后,硫柳汞(EtHg)和无机汞在肾脏中的最大添加浓度出现,为81μg汞/克。EtHg占肾脏汞的59%,无机汞占41%。总之,有机汞化合物硫柳汞(EtHg)具有与甲基汞相似的初始免疫抑制作用。然而,与甲基汞不同的是,硫柳汞处理在基因易感性小鼠中会导致第二阶段出现强烈的免疫刺激和自身免疫,这是T细胞依赖性的、与H-2相关的,并且可能至少部分归因于乙基汞代谢产生的无机汞。

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