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首页> 外文期刊>Journal of the American Society of Nephrology: JASN >Antigen identification in membranous nephropathy moves toward targeted monitoring and new therapy.
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Antigen identification in membranous nephropathy moves toward targeted monitoring and new therapy.

机译:膜肾病中抗原鉴定朝向靶向监测和新疗法。

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Membranous nephropathy, a disease characterized by an accumulation of immune deposits on the outer aspect of the glomerular basement membrane, is the most common cause of idiopathic nephrotic syndrome in Caucasian adults. In the rat model described by Heymann in 1959, the target antigen of antibodies is megalin, a multiligand receptor expressed in the rat glomerulus but absent from the human glomerulus. In the past few years, two major antigens have been identified in human membranous nephropathy. The first is neutral endopeptidase, the alloantigen involved in neonatal cases of membranous nephropathy that occur in newborns from neutral endopeptidase-deficient mothers. The second is the type-M phospholipase A2 receptor (PLA(2)R), the first autoantigen identified in idiopathic membranous nephropathy in the adult. Megalin, neutral endopeptidase, and PLA(2)R are all expressed on the podocyte surface where they serve as targets for circulating antibodies, which lead to in situ immune complex formation, complement activation, and proteinuria. The recent discovery of neutral endopeptidase and PLA(2)R provides new tools for monitoring human disease activity and should be of value in designing new antigen-driven therapeutic strategies.
机译:膜状肾病,一种疾病,其特征在于肾小球基底膜外表的免疫沉积物的积累,是白种人成年人特发性肾病综合征最常见的原因。在1959年的Heymann描述的大鼠模型中,抗体的靶抗原是巨大的,在大鼠肾小球中表达但不存在于人肾小球中的多硅受体。在过去几年中,已经在人膜肾病中鉴定了两种主要抗原。首先是中性内肽酶,血液抗原参与新生儿膜肾病的新生儿病例,其来自中性内肽酶缺乏母亲的新生儿。第二种是M磷脂酶A2受体(PLA(2)R),其在成人特发性膜肾病中鉴定的第一自身抗原。巨脂素,中性内肽酶和PLA(2)R全部表达在孔细胞表面上,它们用作循环抗体的靶标,这导致原位免疫复合物形成,补体激活和蛋白尿。最近的中性内肽酶和PLA(2)R的发现提供了用于监测人类疾病活动的新工具,并且应该具有设计新的抗原驱动的治疗策略的价值。

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