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抗独特型抗体直接干扰肾小球IgA免疫复合物的沉积。

Anti-idiotype antibody directly interferes with glomerular IgA immune complex deposition.

作者信息

Chen A, Sheu L F, Shaio M F, Huang T H, Ding S L, Lee W H

机构信息

Department of Pathology, Tri-Service General Hospital, National Defense Medical Center, Taipei, Taiwan/ROC.

出版信息

Nephron. 1998;78(4):464-73. doi: 10.1159/000044976.

Abstract

Data from both animal and clinical studies suggest that anti-idiotype antibodies deposited in glomeruli may be involved in the pathogenesis of glomerulonephritis. This study was conducted to examine the role of a hybridoma-AB1-2-derived IgG anti-T15 idiotype (IgG anti-T15) in the immunopathogenesis of a short-term experimental IgA nephropathy. BALB/c mice (12/group) were administered intravenously with: (1) an equal mass (1 mg) of T15-hybridoma-derived IgA antiphosphorylcholine (PC) and PC-conjugated bovine serum albumin (BSA-PC) antigen; (2) 1 mg of IgA anti-PC, 1 mg of BSA-PC antigen, and 3 mg of IgG anti-T15, or (3) 1 mg of BSA-PC antigen alone. The mice were sacrificed 6 h after the injection. A 6-hour clearance study was performed. The initial phase of elimination of BSA-PC antigen in mice receiving IgA anti-PC/BSA-PC/IgG anti-T15 or those receiving the antigen alone was significantly faster than that in those receiving IgA anti-PC/BSA-PC (p < 0.001). There was no significant difference in the elimination rate of BSA-PC antigen between mice receiving IgA anti-PC/BSA-PC/IgG anti-T15 and those receiving BSA-PC antigen alone. The late phases of elimination of the BSA-PC antigen in mice receiving IgA anti-PC/BSA-PC/IgG anti-T15 showed somewhat similar to those of BSA-PC antigen in mice receiving IgA anti-PC/BSA-PC. Moreover, mice injected with IgA anti-PC/BSA-PC/IgG anti-T15 showed a significantly less glomerular BSA-PC antigen deposition than those injected with IgA anti-PC/BSA-PC (positive control), as demonstrated by light microscopy, autoradiography, and immunohistochemistry (each p < 0.001). It is inferred that the injected IgG anti-T15 could react with the IgA anti-PC in vivo, directly interfering with immune complex formation by the IgA anti-PC and BSA-PC antigen, thereby resulting in diminished glomerular deposition of the BSA-PC antigen. These findings suggest that an anti-idiotype antibody may be protective in the immunopathogenesis of IgA nephropathy, because of its inhibitory effect on glomerular trapping of an antigen.

摘要

来自动物和临床研究的数据表明,沉积在肾小球中的抗独特型抗体可能参与了肾小球肾炎的发病机制。本研究旨在探讨杂交瘤AB1 - 2衍生的IgG抗T15独特型抗体(IgG抗T15)在短期实验性IgA肾病免疫发病机制中的作用。将BALB/c小鼠(每组12只)静脉注射:(1)等量质量(1毫克)的T15杂交瘤衍生的IgA抗磷酸胆碱(PC)和PC偶联的牛血清白蛋白(BSA - PC)抗原;(2)1毫克IgA抗PC、1毫克BSA - PC抗原和3毫克IgG抗T15,或(3)仅1毫克BSA - PC抗原。注射后6小时处死小鼠。进行了一项6小时的清除研究。接受IgA抗PC/BSA - PC/IgG抗T15的小鼠或仅接受抗原的小鼠中,BSA - PC抗原清除的初始阶段明显快于接受IgA抗PC/BSA - PC的小鼠(p < 0.001)。接受IgA抗PC/BSA - PC/IgG抗T15的小鼠与仅接受BSA - PC抗原的小鼠之间,BSA - PC抗原的清除率没有显著差异。接受IgA抗PC/BSA - PC/IgG抗T15的小鼠中BSA - PC抗原清除的后期阶段与接受IgA抗PC/BSA - PC的小鼠中BSA - PC抗原的后期阶段有些相似。此外,通过光学显微镜、放射自显影和免疫组织化学证实(各p < 0.001),注射IgA抗PC/BSA - PC/IgG抗T15的小鼠肾小球中BSA - PC抗原的沉积明显少于注射IgA抗PC/BSA - PC的小鼠(阳性对照)。据推测,注射的IgG抗T15可在体内与IgA抗PC反应,直接干扰IgA抗PC和BSA - PC抗原形成免疫复合物,从而导致BSA - PC抗原在肾小球中的沉积减少。这些发现表明,抗独特型抗体可能因其对肾小球捕获抗原的抑制作用而在IgA肾病的免疫发病机制中具有保护作用。

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