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抗独特型免疫与自身免疫。I. 针对大鼠甲状腺球蛋白自发产生的自身抗体的抗独特型抗体的体外和体内效应

Anti-idiotypic immunity and autoimmunity. I. In vitro and in vivo effects of anti-idiotypic antibodies to spontaneously occurring autoantibodies to rat thyroglobulin.

作者信息

Zanetti M, Bigazzi P E

出版信息

Eur J Immunol. 1981 Mar;11(3):187-95. doi: 10.1002/eji.1830110306.

Abstract

The effects of anti-receptor (anti-idiotypic) immunity on autoimmune responses have been investigated in Buffalo (BUF) rats with autoimmune thyroiditis. As compared to other animal models of autoimmune disease, BUF rat thyroiditis has the following advantages: it occurs in an inbred strain, arises spontaneously (i.e. without the experimental administration of autoantigens and adjuvants) and is characterized by production of autoantibodies to only one autoantigen, thyroglobulin. Finally, its pathogenesis is mediated by autoantibodies to rat thyroglobulin, and therefore this model is particularly suitable to study the effects of anti-idiotypic reactions on those autoimmune disorders whose damage is caused by humoral immunity. The experiments reported in the present study show that first, heterologous anti-idiotypic antibodies to autoantibodies against rat thyroglobulin have been produced and characterized. It has then been demonstrated that such anti-idiotypic antibodies are capable of inhibiting the in vitro binding between thyroglobulin and thyroglobulin autoantibodies obtained from BUF rats. It has also been shown that repeated injections of anti-idiotypic antibodies into sublethally X-irradiated BUF rats with autoimmune thyroiditis were followed by a significant change in the levels of circulating autoantibodies to rat thyroglobulin. These results provide evidence that in spite of the complexity of autoantigens and the heterogeneity of autoimmune responses, established autoimmune diseases may be controlled by sequential immunosuppression and anti-idiotypic immunity.

摘要

在患有自身免疫性甲状腺炎的布法罗(BUF)大鼠中,研究了抗受体(抗独特型)免疫对自身免疫反应的影响。与其他自身免疫性疾病动物模型相比,BUF大鼠甲状腺炎具有以下优点:它发生在近交系中,自发产生(即无需实验性给予自身抗原和佐剂),并且其特征是仅针对一种自身抗原甲状腺球蛋白产生自身抗体。最后,其发病机制由抗大鼠甲状腺球蛋白自身抗体介导,因此该模型特别适合研究抗独特型反应对那些由体液免疫引起损伤的自身免疫性疾病的影响。本研究报告的实验表明,首先,已制备并鉴定了针对抗大鼠甲状腺球蛋白自身抗体的异源抗独特型抗体。然后证明了这种抗独特型抗体能够抑制甲状腺球蛋白与从BUF大鼠获得的甲状腺球蛋白自身抗体之间的体外结合。还表明,将抗独特型抗体反复注射到患有自身免疫性甲状腺炎的经亚致死剂量X射线照射的BUF大鼠中后,大鼠甲状腺球蛋白循环自身抗体水平发生了显著变化。这些结果证明,尽管自身抗原复杂且自身免疫反应具有异质性,但已确立的自身免疫性疾病可以通过序贯免疫抑制和抗独特型免疫来控制。

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