Rastaldi M P, Candiano G, Musante L, Bruschi M, Armelloni S, Rimoldi L, Tardanico R, Sanna-Cherchi S, Ferrario F, Montinaro V, Haupt R, Parodi S, Carnevali M L, Allegri L, Camussi G, Gesualdo L, Scolari F, Ghiggeri G M
Renal Immunopathology Laboratory, Fondazione D'Amico per la Ricerca sulle Malattie Renali, Nuova Nefrologia Research Association, c/o San Carlo Borromeo Hospital, Milan, Italy.
Kidney Int. 2006 Aug;70(3):477-85. doi: 10.1038/sj.ki.5001563. Epub 2006 Jun 14.
Mechanisms for human membranous glomerulonephritis (MGN) remain elusive. Most up-to-date concepts still rely on the rat model of Passive Heymann Nephritis that derives from an autoimmune response to glomerular megalin, with complement activation and membrane attack complex assembly. Clusterin has been reported as a megalin ligand in immunodeposits, although its role has not been clarified. We studied renal biopsies of 60 MGN patients by immunohistochemistry utilizing antibodies against clusterin, C5b-9, and phosphorylated-protien kinase C (PKC) isoforms (pPKC). In vitro experiments were performed to investigate the role of clusterin during podocyte damage by MGN serum and define clusterin binding to human podocytes, where megalin is known to be absent. Clusterin, C5b-9, and pPKC-alpha/beta showed highly variable glomerular staining, where high clusterin profiles were inversely correlated to C5b-9 and PKC-alpha/beta expression (P=0.029), and co-localized with the low-density lipoprotein receptor (LDL-R). Glomerular clusterin emerged as the single factor influencing proteinuria at multivariate analysis and was associated with a reduction of proteinuria after a follow-up of 1.5 years (-88.1%, P=0.027). Incubation of podocytes with MGN sera determined strong upregulation of pPKC-alpha/beta that was reverted by pre-incubation with clusterin, serum de-complementation, or protein-A treatment. Preliminary in vitro experiments showed podocyte binding of biotinilated clusterin, co-localization with LDL-R and specific binding inhibition with anti-LDL-R antibodies and with specific ligands. These data suggest a central role for glomerular clusterin in MGN as a modulator of inflammation that potentially influences the clinical outcome. Binding of clusterin to the LDL-R might offer an interpretative key for the pathogenesis of MGN in humans.
人类膜性肾小球肾炎(MGN)的发病机制仍不清楚。大多数最新概念仍依赖于被动性海曼肾炎大鼠模型,该模型源于对肾小球megalin的自身免疫反应,伴有补体激活和膜攻击复合物组装。尽管尚未阐明其作用,但聚集素已被报道为免疫沉积物中的一种megalin配体。我们利用抗聚集素、C5b-9和磷酸化蛋白激酶C(PKC)亚型(pPKC)的抗体,通过免疫组织化学研究了60例MGN患者的肾活检标本。进行了体外实验,以研究聚集素在MGN血清导致的足细胞损伤中的作用,并确定聚集素与人足细胞的结合情况,已知人足细胞中不存在megalin。聚集素、C5b-9和pPKC-α/β显示出高度可变的肾小球染色,其中高聚集素水平与C5b-9和PKC-α/β表达呈负相关(P=0.029),并与低密度脂蛋白受体(LDL-R)共定位。在多变量分析中,肾小球聚集素成为影响蛋白尿的单一因素,并且在随访1.5年后与蛋白尿减少相关(-88.1%,P=0.027)。用MGN血清孵育足细胞可导致pPKC-α/β强烈上调,而预先用聚集素孵育、血清去补体或蛋白A处理可使其恢复。初步体外实验显示生物素化聚集素与足细胞结合,与LDL-R共定位,并被抗LDL-R抗体和特异性配体特异性抑制结合。这些数据表明肾小球聚集素在MGN中作为炎症调节剂具有核心作用,可能影响临床结局。聚集素与LDL-R的结合可能为人类MGN发病机制提供一个解释关键。
