Asanuma Katsuhiko, Mundel Peter
Division of Nephrology, Albert Einstein College of Medicine, 1300 Morris Park Avenue, Bronx, NY 10461, USA.
Clin Exp Nephrol. 2003 Dec;7(4):255-9. doi: 10.1007/s10157-003-0259-6.
Podocytes are unique cells with a complex cellular organization. With respect to their cytoarchitecture, podocytes may be divided into three structurally and functionally different segments: cell body, major processes, and foot processes (FPs). The FPs of neighboring podocytes regularly interdigitate, leaving between them the filtration slits that are bridged by an extracellular structure, known as the slit diaphragm (SD). Podocytes cover the outer aspect of the glomerular basement membrane (GBM). They therefore form the final barrier to protein loss, which explains why podocyte injury is typically associated with marked proteinuria. Chronic podocyte injury may lead to podocyte detachment from the GBM. Our knowledge of the molecular structure of the SD has been remarkably improved in the past few years. Several molecules, including nephrin, CD2AP, FAT, ZO-1, P-cadherin, Podocin, and Neph 1-3 have all been shown to be associated with the SD complex, and some of these molecules are critical for its integrity. Podocytes are injured in many forms of human and experimental glomerular disease. The early events are characterized either by alterations in the molecular composition of the SD without visible changes in morphology or, more obviously, by a reorganization of FP structure with the fusion of filtration slits and the apical displacement of the SD. Based on recent insights into the molecular pathology of podocyte injury, at least four major causes have been identified that lead to the uniform reaction of FP effacement and proteinuria: (1) interference with the SD complex and its lipid rafts; (2) direct interference with the actin cytoskeleton; (3) interference with the GBM or with podocyte-GBM interaction; and (4) interference with the negative surface charge of podocytes. There is also evidence, in focal segmental glomerular sclerosis (FSGS) and in idiopathic nephrotic syndrome in humans and rats, that podocyte damage may be caused by circulating albuminuric factors. Ongoing studies in many laboratories are aiming at an understanding of the dynamic relationship between SD proteins, the actin cytoskeleton, and the dynamics of FP structure in nephrotic syndrome and FSGS. These studies should provide us with a better understanding of the biological mechanism underlying the podocyte response to injury. Such studies will potentially translate into more refined treatment and the prevention of proteinuria and progressive glomerular disease.
足细胞是具有复杂细胞结构的独特细胞。就其细胞结构而言,足细胞可分为三个结构和功能不同的部分:细胞体、主突和足突(FP)。相邻足细胞的足突经常相互交错,在它们之间留下由一种称为裂孔隔膜(SD)的细胞外结构桥接的滤过裂隙。足细胞覆盖肾小球基底膜(GBM)的外表面。因此,它们形成了防止蛋白质丢失的最后一道屏障,这就解释了为什么足细胞损伤通常与明显的蛋白尿有关。慢性足细胞损伤可能导致足细胞与GBM分离。在过去几年中,我们对SD分子结构的了解有了显著提高。包括nephrin、CD2AP、FAT、ZO-1、P-钙黏蛋白、Podocin和Neph 1-3在内的几种分子都已被证明与SD复合体有关,其中一些分子对其完整性至关重要。在许多形式的人类和实验性肾小球疾病中,足细胞都会受到损伤。早期事件的特征要么是SD分子组成的改变而形态无明显变化,要么更明显的是FP结构的重组,伴有滤过裂隙融合和SD的顶端移位。基于对足细胞损伤分子病理学的最新认识,已确定至少有四个主要原因导致FP消失和蛋白尿的一致反应:(1)干扰SD复合体及其脂筏;(2)直接干扰肌动蛋白细胞骨架;(3)干扰GBM或足细胞与GBM的相互作用;(4)干扰足细胞的负表面电荷。在人类和大鼠的局灶节段性肾小球硬化(FSGS)和特发性肾病综合征中也有证据表明,足细胞损伤可能是由循环中的蛋白尿因子引起的。许多实验室正在进行的研究旨在了解肾病综合征和FSGS中SD蛋白、肌动蛋白细胞骨架与FP结构动力学之间的动态关系。这些研究将使我们更好地理解足细胞对损伤反应的生物学机制。此类研究可能会转化为更精细的治疗方法以及预防蛋白尿和进行性肾小球疾病。
