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转基因编码的IgG2b自身抗体的组成性分泌导致自身免疫性疾病症状。

Constitutive secretion of transgene-encoded IgG2b autoantibodies leads to symptoms of autoimmune disease.

作者信息

Radic M Z, Ibrahim S M, Rauch J, Camper S A, Weigert M

机构信息

Department of Microbiology and Immunology, Medical College of Pennsylvania, Philadelphia 19129, USA.

出版信息

J Immunol. 1995 Sep 15;155(6):3213-22.

PMID:7673734
Abstract

Anti-DNA Ab are strictly regulated, except in autoimmunity, where they are expressed and may contribute to pathogenicity. To study constitutive anti-DNA Ab secretion in nonautoimmune mice, two anti-dsDNA H/L chain transgene combinations were constructed using an IgG2b C region with secretory but no transmembrane domain exons. One H/L combination, consisting of the VH3H9 H and V kappa 4 L chain transgenes, was chosen to recreate 3H9, an autoantibody that originally arose in an autoimmune MRL/lpr mouse; the other paired a higher affinity variant of VH3H9, 56R, with the same V kappa 4 L chain. Elevated titers of IgG2b along with normal levels of other isotypes were observed in transgene-positive mice, indicating that constitutive transgene-directed Ab secretion was achieved. Sera and hybridoma supernatants from VH3H9 gamma transgene-positive animals exhibited binding to dsDNA, ssDNA, and cardiolipin. Mice expressing the 56R gamma H chain and the V kappa 4 L chain showed enhanced binding. Expression of the transgenes correlated with signs of autoimmune disease, including prolonged plasma clotting in vitro, and reduced litter size. The results suggest that even a single autoreactive H chain that escapes tolerance may suffice to induce features of autoimmune disease.

摘要

抗DNA抗体受到严格调控,自身免疫情况除外,在自身免疫中它们会表达并可能导致致病性。为了研究非自身免疫小鼠中组成型抗DNA抗体的分泌情况,使用具有分泌但无跨膜结构域外显子的IgG2b C区构建了两种抗双链DNA重链/轻链转基因组合。选择一种重链/轻链组合,由VH3H9重链和Vκ4轻链转基因组成,以重现最初出现在自身免疫性MRL/lpr小鼠中的自身抗体3H9;另一种将VH3H9的高亲和力变体56R与相同的Vκ4轻链配对。在转基因阳性小鼠中观察到IgG2b滴度升高以及其他同种型水平正常,表明实现了组成型转基因导向的抗体分泌。来自VH3H9γ转基因阳性动物的血清和杂交瘤上清液表现出与双链DNA、单链DNA和心磷脂的结合。表达56Rγ重链和Vκ4轻链的小鼠显示出增强的结合。转基因的表达与自身免疫性疾病的迹象相关,包括体外血浆凝血时间延长和窝仔数减少。结果表明,即使是一个逃避耐受的自身反应性重链也可能足以诱发自身免疫性疾病的特征。

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