Rose N R, Rasooly L, Saboori A M, Burek C L
Department of Molecular Microbiology and Immunology, The Johns Hopkins Medical Institutions, Baltimore, MD 21205, USA.
Environ Health Perspect. 1999 Oct;107 Suppl 5(Suppl 5):749-52. doi: 10.1289/ehp.99107s5749.
A great deal of circumstantial evidence has linked iodine with the rising incidence of autoimmune thyroiditis in the United States. In our investigations, we have shown directly that T cells from humans with chronic lymphocytic thyroiditis proliferate in the presence of iodinated but not in the presence of noniodinated human thyroglobulin. Moreover, the proliferative response is restored when the thyroglobulin is iodinated artificially in vitro. Using a panel of monoclonal antibodies, we found evidence that the presence of iodine induces a number of stereochemical changes in the conformation of the molecule, resulting in the loss of some antigenic determinants and the appearance of others. One prominent determinant was associated with the iodine-containing amino acid thyroxine. Both the number and position of the iodine substituents determine the precise specificity of this epitope. A new model for the study of the role of iodine in inducing thyroid autoimmunity has become available in the form of the nonobese diabetic (NOD)-H2(h4) mouse. This animal develops autoimmune thyroiditis spontaneously but in relatively low prevalence. However, if iodine is added to the drinking water, the prevalence and severity of the thyroid lesions increase markedly. The immune response is specific for thyroglobulin, both in terms of the antibody response and T-cell proliferation. In fact, the appearance of lesions can be predicted by the presence of thyroglobulin-specific IgG2b antibody. The disease, moreover, can be transferred adoptively, using spleen cells from iodine-fed donors treated in vitro with iodinated thyroglobulin. The effects of iodine feeding are greater in conventional animals compared with those maintained under specific pathogen-free conditions. Based on T-cell proliferation, it appears that the NOD-H2(h4) strain of mice has innately a greater response to murine thyroglobulin than do other mouse strains and that the proliferation is increased even more by feeding iodine. We suggest, therefore, that the presence of iodine increases the autoantigenic potency of thyroglobulin, a major pathogenic antigen in the induction of autoimmune thyroiditis. This animal model provides a unique opportunity for investigating in detail the mechanisms by which an environmental agent can trigger a pathogenic autoimmune response in a susceptible host.
大量间接证据表明,在美国,碘与自身免疫性甲状腺炎发病率的上升有关。在我们的研究中,我们直接表明,患有慢性淋巴细胞性甲状腺炎的人的T细胞在碘化人甲状腺球蛋白存在的情况下会增殖,而在非碘化人甲状腺球蛋白存在的情况下则不会增殖。此外,当甲状腺球蛋白在体外人工碘化时,增殖反应得以恢复。使用一组单克隆抗体,我们发现有证据表明碘的存在会导致分子构象发生一些立体化学变化,从而导致一些抗原决定簇的丧失和其他抗原决定簇的出现。一个突出的决定簇与含碘氨基酸甲状腺素有关。碘取代基的数量和位置决定了这个表位的精确特异性。一种以非肥胖糖尿病(NOD)-H2(h4)小鼠形式存在的研究碘在诱导甲状腺自身免疫中作用的新模型已经可用。这种动物会自发发生自身免疫性甲状腺炎,但发病率相对较低。然而,如果在饮用水中添加碘,甲状腺病变的发病率和严重程度会显著增加。无论是在抗体反应还是T细胞增殖方面,免疫反应都是针对甲状腺球蛋白的。事实上,病变的出现可以通过甲状腺球蛋白特异性IgG2b抗体的存在来预测。此外,使用来自经碘化甲状腺球蛋白体外处理的碘喂养供体的脾细胞,可以过继转移这种疾病。与在无特定病原体条件下饲养的动物相比,在常规动物中碘喂养的效果更大。基于T细胞增殖,似乎NOD-H2(h4)小鼠品系对鼠甲状腺球蛋白天生就比其他小鼠品系有更大的反应,并且通过喂养碘,增殖会进一步增加。因此,我们认为碘的存在会增加甲状腺球蛋白的自身抗原效力,甲状腺球蛋白是诱导自身免疫性甲状腺炎的主要致病抗原。这个动物模型为详细研究环境因素如何在易感宿主中引发致病性自身免疫反应的机制提供了独特的机会。