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首页> 外文期刊>Clinical and Experimental Immunology: An Official Journal of the British Society for Immunology >Spreading of antibody reactivity to non-thyroid antigens during experimental immunization with human thyroglobulin.
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Spreading of antibody reactivity to non-thyroid antigens during experimental immunization with human thyroglobulin.

机译:在用人甲状腺球蛋白进行实验性免疫期间,抗体对非甲状腺抗原的反应性扩散。

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Intermolecular spreading of antibody reactivity has been implicated in the evolution of autoimmune disease. In this study, spreading of antibody reactivity to non-thyroid autoantigens after experimental immunization with thyroglobulin (Tg) was investigated. For this purpose, two rabbits were injected with human Tg six times (stages 1-6) every 3 weeks. Animals were also bled before priming. Antisera were tested by enzyme-linked immunosorbent assay (ELISA) for reactivity to several non-thyroid antigens: bovine serum albumin (BSA), native DNA (nDNA), human myosin, human globular (G) and filamentous (F) actin and porcine tubulin. Tg-immunized animals developed the following serological reactivity pattern: (a) high reactivity to myosin from stage 2 onward, (b) significant reactivity to F-actin, remaining high up to stage 6, (c) reactivity to BSA with a peak at stage 3, (d) a small increase of reactivity to G-actin at stage 3 and (e) no increase of reactivity to nDNA and tubulin. The study of affinity-purified anti-Tg antibodies and the use of competitive assays revealed that reactivity to F-actin was not due to cross-reaction with Tg. On the contrary, reactivity to myosin during the first stages of immunization was due to cross-reaction with Tg, while at stage 6 it became myosin-specific. Reactivity to BSA at stage 3 was also due to cross-reaction with Tg. We conclude that at least part of the induced anti-Tg antibodies may result from the expansion of B cell clones producing polyreactive natural autoantibodies, and polyreactivity of anti-Tg antibodies during the first stages of Tg-immunization may be responsible for the intermolecular spreading of antibody response.
机译:抗体反应性的分子间扩散与自身免疫疾病的发展有关。在这项研究中,研究了甲状腺球蛋白(Tg)实验性免疫后抗体对非甲状腺自身抗原的反应性传播。为此,每三周向两只兔子注射人Tg六次(1-6阶段)。在启动前也将动物放血。通过酶联免疫吸附测定(ELISA)测试抗血清对几种非甲状腺抗原的反应性:牛血清白蛋白(BSA),天然DNA(nDNA),人肌球蛋白,人球状(G)和丝状(F)肌动蛋白和猪微管蛋白。经Tg免疫的动物发展出以下血清学反应性模式:(a)从第2阶段开始对肌球蛋白有高反应性,(b)对F-肌动蛋白有显着反应性,直至第6阶段仍保持高反应性,(c)对BSA的反应性达到峰值在第3阶段,(d)在第3阶段对G-肌动蛋白的反应性略有增加,以及(e)对nDNA和微管蛋白的反应性没有增加。对亲和纯化的抗Tg抗体的研究和竞争性分析的使用表明,对F-肌动蛋白的反应性不是由于与Tg的交叉反应。相反,在免疫的第一阶段与肌球蛋白的反应性是由于与Tg的交叉反应,而在第6阶段,它变成了肌球蛋白特异性的。在阶段3与BSA的反应性也归因于与Tg的交叉反应。我们得出的结论是,至少部分诱导的抗Tg抗体可能是由产生多反应性天然自身抗体的B细胞克隆的扩增引起的,并且在Tg免疫的第一阶段,抗Tg抗体的多反应性可能是导致Tg分子间扩散的原因。抗体反应。

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