New antigens involved in membranous nephropathy beyond phospholipase A2 receptor.

Maurizio Salvadori, Aris Tsalouchos
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引用次数: 2

Abstract

When the physiopathology of membranous nephropathy was first described, almost 30% of cases were recognized to be secondary to well-known diseases such as autoimmune diseases, tumors or infections. The remaining 70% cases were called primary membranous nephropathy as the exact mechanism or pathogenic factor involved was unknown. The discovery of the M type phospholipase A2 receptor and thrombospondin type 1 domain containing 7A as causative antigens in these "so called" primary membranous nephropathies provided new insights into the effective causes of a large proportion of these cases. Novel techniques such as laser microdissection and tandem mass spectrometry as well as immunochemistry with antibodies directed against novel proteins allowed the confirmation of new involved antigens. Finally, using confocal microscopy to localize these new antigens and immunoglobulin G and Western blot analysis of serum samples, these new antigens were detected on the glomerular membrane, and the related antibodies were detected in serum samples. The same antigens have been recognized in some cases of secondary membranous disease due to autoimmune diseases, tumors and infections. This has allowed examination of the relationship between antigens in primary membranous nephropathy and their presence in some secondary nephropathies. The aim of this study is to describe the characteristics of the new antigens discovered and their association with other diseases.

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磷脂酶A2受体以外参与膜性肾病的新抗原。
当膜性肾病的生理病理首次被描述时,几乎30%的病例被认为是继发于众所周知的疾病,如自身免疫性疾病、肿瘤或感染。其余70%的病例被称为原发性膜性肾病,因为确切的机制或致病因素尚不清楚。在这些“所谓的”原发性膜性肾病中发现M型磷脂酶A2受体和含有7A的血栓反应蛋白1型结构域作为致病抗原,为这些病例的大部分有效病因提供了新的见解。新的技术,如激光显微解剖和串联质谱,以及针对新蛋白质的抗体免疫化学,使得新的抗原得以确认。最后利用共聚焦显微镜对这些新抗原进行定位,并对血清样品进行免疫球蛋白G和Western blot分析,在肾小球膜上检测到这些新抗原,并在血清样品中检测到相关抗体。在一些由自身免疫性疾病、肿瘤和感染引起的继发性膜性疾病中也发现了相同的抗原。这允许检查抗原在原发性膜性肾病和他们的存在在一些继发性肾病之间的关系。本研究的目的是描述新发现的抗原的特征及其与其他疾病的关系。
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