Regele Heinrich M, Fillipovic Edith, Langer Brigitte, Poczewki Helga, Kraxberger Ilse, Bittner Reginald E, Kerjaschki Dontscho
Institute for Clinical Pathology, University of Vienna, Allgemeines Krankenhaus, Austria.
Institute of Anatomy, Neuromuscular Research Department, University of Vienna, Vienna, Austria.
J Am Soc Nephrol. 2000 Mar;11(3):403-412. doi: 10.1681/ASN.V113403.
Extensive flattening of podocyte foot processes and increased permeability of the glomerular capillary filter are the major pathologic features of minimal change nephrosis (MCN) and focal segmental glomerulosclerosis (FSGS). Adhesion proteins anchor and stabilize podocytes on the glomerular basement membrane (GBM), and presumably are involved in the pathogenesis of foot process flattening. Thus far, ao3 P,-integrin was localized to basal cell membrane domains. In this report, ao- and 3-dystroglycan (DG) were detected at precisely the sa-ne location by immunoelectron microscopy. and the presence of ac- and /-DG chains was confirmed by immunoblotting on isolated human glomeruli. Because the major DG binding partners in the GBM (laminin, agrin, perlecan), and the intracellular dystrophin analogue utrophin are also present in glomeruli, it appears that podocytes adhere to the GBM via DG complexes, similar to muscle fibers in which actin is linked via dystrophin and DG to the extracellular matrix. As with muscle cells, it is therefore plausible that podocytes use precisely actin-guided DG complexes at their "soles" to actively govern the topography of GBM matrix proteins. Expression of the a//3-DG complex was reported to be reduced in muscular dystrophies. and therefore a search for similar pathologic alterations in archival kidney biopsies from patients with MCN (it = 16) and FSGS (ni = 8) was conducted by quantitative immunoelectron microscopy. The density of a-DG on the podocyte's soles was significantly reduced to 25% in MCN, whereas it was not different in normal kidneys and FSGS. The expression of 3-DG was reduced to >50% in MCN, and was slightly increased in FSGS. Levels of DG expression returned to normal in MCN after steroid treatment (7 = 4). Expression of /3-integrin remained at normal levels in all conditions. These findings point to different potentially pathogenic mechanisms of foot process flattening in MCN and FSGS.
足细胞足突广泛扁平以及肾小球滤过膜通透性增加是微小病变性肾病(MCN)和局灶节段性肾小球硬化(FSGS)的主要病理特征。黏附蛋白将足细胞锚定并稳定在肾小球基底膜(GBM)上,推测其参与了足突扁平的发病机制。到目前为止,α3β1-整合素定位于基底细胞膜结构域。在本报告中,通过免疫电子显微镜在精确相同的位置检测到了α-和β-肌营养不良聚糖(DG),并且通过对分离的人肾小球进行免疫印迹证实了α-和β-DG链的存在。由于GBM中主要的DG结合伴侣(层粘连蛋白、聚集蛋白、基底膜聚糖)以及细胞内肌营养不良蛋白类似物桥粒蛋白也存在于肾小球中,似乎足细胞通过DG复合物黏附于GBM,类似于肌纤维中肌动蛋白通过肌营养不良蛋白和DG与细胞外基质相连。因此,与肌肉细胞一样,足细胞在其“底部”精确地利用肌动蛋白引导的DG复合物来主动控制GBM基质蛋白的拓扑结构是合理的。据报道,α/β-DG复合物的表达在肌肉营养不良中降低,因此通过定量免疫电子显微镜对MCN患者(n = 16)和FSGS患者(n = 8)的存档肾活检组织进行了类似病理改变的研究。MCN中足细胞底部α-DG的密度显著降低至正常肾脏和FSGS的25%,而在正常肾脏和FSGS中无差异。MCN中β-DG的表达降低至>50%,而在FSGS中略有增加。类固醇治疗后(n = 4),MCN中DG的表达水平恢复正常。在所有情况下,β-整合素的表达保持在正常水平。这些发现指出了MCN和FSGS中足突扁平不同的潜在致病机制。
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