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用葡萄球菌磷酸酶诱导大鼠肾小球肾炎:感染后免疫复合物性肾小球肾炎的新方面

Induction of glomerulonephritis in rats with staphylococcal phosphatase: new aspects in post-infectious ICGN.

作者信息

Yousif Y, Okada K, Batsford S, Vogt A

机构信息

Department of Immunology, Institute of Medical Microbiology, Freiburg University, Germany.

出版信息

Kidney Int. 1996 Jul;50(1):290-7. doi: 10.1038/ki.1996.314.

Abstract

Staphylococcal neutral phosphatase (NPtase) is a highly cationic bacterial surface bound protein. It has significant affinity for human and rat immunoglobulins in vitro and an electrostatic interaction may be involved. Radioisotopic studies showed that NPtase had a high affinity for the polyanionic structures of the rat renal glomerulus. When the left kidneys of germ-free or naive (non-immune) Wistar rats were perfused with 80 micrograms of I125 NPtase, 21 micrograms of NPtase were found in the left kidneys and 11 micrograms in the isolated glomeruli 15 minutes after perfusion. Deposits of autologous immunoglobulin and C3 were seen in the glomeruli of rats immediately after perfusion with NPtase (15 min) and persisted throughout the 14-day observation period. Histologically, neutrophil influx into the glomerulus was seen at 15 minutes and increased until three hours; subepithelial electron-dense deposits were found after three days and were still visible on day 14. Proteinuria started within the first 24 hours despite the absence of an immune response at this time and was still present on day 14. Similar results were observed in immune deficient athymic nude rats in the early phase. Perfusion of heparin after NPtase inhibited the deposition of IgG and C3 and prevented proteinuria in naive but not in actively immunized rats. This result provides further evidence that specific antibodies to NPtase were not involved in the immune complex-like deposits seen in the early phase. NPtase is a novel molecule, as it reveals both high affinity for the GBM and binding of circulating immunoglobulins, by a non-antigen-antibody mechanism, to form IC-like deposits on the GBM. These deposits are capable of activating the complement system, thus triggering a series of events leading to glomerulonephritis. These results delineate an additional pathway for the pathogenesis of ICGN related to bacterial infection.

摘要

葡萄球菌中性磷酸酶(NPtase)是一种高度带阳离子电荷的细菌表面结合蛋白。它在体外对人和大鼠免疫球蛋白具有显著亲和力,可能涉及静电相互作用。放射性同位素研究表明,NPtase对大鼠肾小球的多阴离子结构具有高亲和力。当用80微克的I125 NPtase灌注无菌或未免疫(非免疫)Wistar大鼠的左肾时,灌注后15分钟在左肾中发现21微克的NPtase,在分离的肾小球中发现11微克。在用NPtase灌注后立即(15分钟)在大鼠肾小球中可见自体免疫球蛋白和C3的沉积,并在整个14天观察期内持续存在。组织学上,在15分钟时可见中性粒细胞流入肾小球,并持续增加直至3小时;3天后发现上皮下电子致密沉积物,在第14天仍可见。尽管此时没有免疫反应,但蛋白尿在最初24小时内开始出现,并在第14天仍然存在。在免疫缺陷的无胸腺裸鼠的早期也观察到类似结果。在NPtase灌注后灌注肝素可抑制IgG和C3的沉积,并预防未免疫大鼠的蛋白尿,但不能预防主动免疫大鼠的蛋白尿。该结果进一步证明,针对NPtase的特异性抗体不参与早期所见的免疫复合物样沉积物。NPtase是一种新分子,因为它既显示出对肾小球基底膜(GBM)的高亲和力,又通过非抗原 - 抗体机制与循环免疫球蛋白结合,在GBM上形成IC样沉积物。这些沉积物能够激活补体系统,从而引发一系列导致肾小球肾炎的事件。这些结果描绘了与细菌感染相关的免疫复合物性肾小球肾炎(ICGN)发病机制的另一条途径。

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