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致肾炎抗体的特异性。III. 抗Fx1A抗体在肾小球中的结合取决于双重特异性。

The specificity of nephritogenic antibodies. III. Binding of anti-Fx1A antibodies in glomeruli is dependent on dual specificity.

作者信息

Bagchus W M, Vos J T, Hoedemaeker P J, Bakker W W

出版信息

Clin Exp Immunol. 1986 Mar;63(3):639-47.

Abstract

Rabbit antibodies against rat tubular brushborder antigens (Fx1A) give rise to in situ formation of immune aggregates along the glomerular capillary walls after intravenous injection into rats. These antibodies (anti-Fx1A), able to produce heterologous immune complex glomerulopathy (HIC) in the rat, have previously been shown to bind with brushborders (anti-BB) as well as with rat thymocytes (anti-T). In the present communication, this dual specificity was also demonstrated in antibodies eluted from kidneys of rats with HIC. It further appeared that, when the anti-thymocyte binding activity was selectively removed from these antibodies, using immunoabsorption with rat tissue extracts, these anti-Fx1A antibodies were no longer able to stain glomerular basement membranes (GBM) as demonstrated at the ultrastructural level using the peroxidase technique. Following perfusion of these antibodies in the normal rat kidney ex vivo, binding along the capillary walls was also below the detection level, in contrast to non anti-T depleted anti-Fx1A IgG. Biochemical analysis (including immunoblotting) showed that the anti-T moiety of anti-Fx1A was directed to a 90 kD component of Fx1A, since selective absorption of this specificity prevented staining of this 90 kD component. It is concluded, that this anti-T specificity within rabbit anti-Fx1A plays a crucial role in local immune complex formation in the rat kidney ex vivo. Whether this holds also for its role in the pathogenesis of HIC in vivo awaits further confirmation.

摘要

针对大鼠肾小管刷状缘抗原(Fx1A)的兔抗体,在静脉注射到大鼠体内后,会沿着肾小球毛细血管壁原位形成免疫聚集体。这些抗体(抗Fx1A)能够在大鼠体内产生异种免疫复合物肾小球病(HIC),此前已证明它们既能与刷状缘(抗BB)结合,也能与大鼠胸腺细胞(抗T)结合。在本报告中,从患有HIC的大鼠肾脏中洗脱的抗体也显示出这种双重特异性。进一步发现,当使用大鼠组织提取物进行免疫吸附,从这些抗体中选择性去除抗胸腺细胞结合活性时,这些抗Fx1A抗体不再能够像使用过氧化物酶技术在超微结构水平上所显示的那样,对肾小球基底膜(GBM)进行染色。在离体的正常大鼠肾脏中灌注这些抗体后,与未去除抗T的抗Fx1A IgG相比,沿毛细血管壁的结合也低于检测水平。生化分析(包括免疫印迹)表明,抗Fx1A的抗T部分针对Fx1A的一个90 kD成分,因为这种特异性的选择性吸附阻止了该90 kD成分的染色。得出的结论是,兔抗Fx1A中的这种抗T特异性在离体大鼠肾脏局部免疫复合物形成中起关键作用。这在体内HIC发病机制中的作用是否也如此,尚待进一步证实。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6638/1577548/95d9a654a2f2/clinexpimmunol00126-0160-a.jpg

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