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通过给予外源性阳离子抗原诱导家兔膜性肾病。

Induction of membranous nephropathy in rabbits by administration of an exogenous cationic antigen.

作者信息

Border W A, Ward H J, Kamil E S, Cohen A H

出版信息

J Clin Invest. 1982 Feb;69(2):451-61. doi: 10.1172/jci110469.

Abstract

We examined the role of antigenic electrical charge as a determinant of glomerular immune complex localization in the rabbit. Serum sickness nephritis was induced in groups of New Zealand white rabbits by daily 25-mg intravenous injections of bovine serum albumin (BSA) chemically modified to be cationic (pI > 9.5) or more anionic (pI, 3.5-4.6); an additional group received unmodified native BSA (pI, 4.5-5.1). Factors known to influence immune complex localization, e.g., molecular size of the administered antigen and resulting circulating immune complexes, immunogenicity, and disappearance time from the circulation were examined and found to be similar for both anionic and cationic BSA. Charge modification did increase the nonimmune clearance of cationic and anionic BSA compared with native BSA. Injected cationic BSA was shown in paired label experiments to bind directly to glomeruli compared with native BSA. The renal lesion produced by cationic BSA was markedly different from that found in rabbits given anionic or native BSA. Animals receiving cationic BSA uniformly developed generalized diffuse granular capillary wall deposits of IgG, C3, and BSA detected after 2 wk of injections and increasing until death at 6 wk. Qualitatively similar deposits were produced by the administration of low doses of cationic BSA of only 1 or 10 mg/d. In contrast, the injection of both anionic and native BSA resulted in mesangial deposits at 2 and 4 wk with capillary wall deposits appearing by 6 wk. Ultrastructural examination of animals receiving cationic BSA revealed pure, extensive formation of dense deposits along the lamina rara externa of the glomerular basement membrane whereas such deposits were absent or rare in animals injected with the anionic or native BSA. Albuminuria was significantly greater at 6 wk in the groups receiving cationic BSA with a mean of 280 mg/24 h compared with 53 mg/24 h in the combined groups injected with anionic or native BSA. Blood urea nitrogen values were similar in all groups at 2 and 4 wk but higher in the animals receiving cationic BSA at 6 wk. These experiments describe the reproducible induction of epimembranous immune deposits by administration of an exogenous cationic antigen. They suggest that antigenic charge can play an important role in the pathogenesis of membranous nephropathy by permitting direct glomerular binding of an antigen and predisposing to in situ immune complex formation.

摘要

我们研究了抗原电荷作为兔肾小球免疫复合物定位决定因素的作用。通过每日静脉注射25毫克化学修饰为阳离子型(pI>9.5)或更阴离子型(pI,3.5 - 4.6)的牛血清白蛋白(BSA),诱导新西兰白兔组发生血清病肾炎;另一组接受未修饰的天然BSA(pI,4.5 - 5.1)。研究了已知影响免疫复合物定位的因素,如所给予抗原和由此产生的循环免疫复合物的分子大小、免疫原性以及从循环中的消失时间,发现阴离子型和阳离子型BSA在这些方面相似。与天然BSA相比,电荷修饰确实增加了阳离子型和阴离子型BSA的非免疫清除率。在配对标记实验中显示,与天然BSA相比,注射的阳离子型BSA直接与肾小球结合。阳离子型BSA产生的肾损伤与给予阴离子型或天然BSA的兔子中发现的损伤明显不同。接受阳离子型BSA的动物在注射2周后均出现IgG、C3和BSA的全身性弥漫性颗粒状毛细血管壁沉积物,并持续增加直至6周死亡。给予仅1或10毫克/天的低剂量阳离子型BSA也产生了定性相似的沉积物。相比之下,注射阴离子型和天然BSA在2周和4周时导致系膜沉积物,6周时出现毛细血管壁沉积物。对接受阳离子型BSA的动物进行超微结构检查发现,沿肾小球基底膜外疏松层有大量纯致密沉积物形成,而在注射阴离子型或天然BSA的动物中,此类沉积物不存在或很少见。接受阳离子型BSA的组在6周时蛋白尿明显更严重,平均为280毫克/24小时,而注射阴离子型或天然BSA的联合组为53毫克/24小时。所有组在2周和4周时血尿素氮值相似,但接受阳离子型BSA的动物在6周时更高。这些实验描述了通过给予外源性阳离子抗原可重复性诱导膜性免疫沉积物。它们表明抗原电荷在膜性肾病的发病机制中可能起重要作用,通过允许抗原直接与肾小球结合并易发生原位免疫复合物形成。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f51a/370995/2a85a1fdce3a/jcinvest00478-0209-a.jpg

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