Nagata M, Kriz W
Institut für Anatomie und Zellbiologie Universität Heidelberg, Germany.
Kidney Int. 1992 Jul;42(1):148-60. doi: 10.1038/ki.1992.272.
In a preceding study [1], we showed that within six months after UNX in young rats, glomeruli in the remnant kidney undergo a sequence of serious changes which finally lead to focal segmental glomerulosclerosis (FGS). The formation of abnormally-shaped capillary channels was shown to result from local mesangial failure and is considered to be a nidus for the development of more severe lesions. In the present paper, the development of characteristic lesions in podocyte structure is described and analyzed. Concomitant with overall glomerular growth after UNX, a pronounced hypertrophy of podocytes was observed, while the mean number of podocytes per glomerulus did not change. It appears that podocytes cannot sustain the same degree of growth as the tuft as a whole; podocyte hypertrophy is soon followed by maladaptive changes which eventually lead to cell destruction. The following sequence of pathologic changes can be suggested: cell bodies enlarge in volume and area associated with a dramatic attenuation to cytoplasmic sheets. Primary processes are thinned out and frequently extend to remote capillaries. As a whole, the capillary area served by a single podocyte is dramatically enlarged. Furthermore, the expanding cytoplasmic sheets (derived from podocyte cell bodies) cover an increasingly large proportion of the outer capillary surface, that is, of the filtration area. Consequently, an increasing amount of filtrate is delivered into the subcellbody space. Obstruction of the efflux of this filtrate into the urinary space causes bulging of the overlying cytoplasmic sheets into pseudocysts. Podocytes overlying abnormally-shaped and dilated capillary channels are generally the most seriously affected. Tuft hypertrophy, pseudocyst formation and local capillary expansion cause wide-spread apposition of podocytes to Bowman's capsule. Appositions are a prerequisite for the development of tuft adhesion. Local detachment of a podocyte from the GBM in those areas allows access of parietal cells to the GBM. In early adhesions the connection of the tuft to Bowman's capsule is established by single parietal cells which attach to both the GBM and the basement membrane of Bowman's capsule. An adhesion is considered as a nidus for segmental sclerosis; as the adhesion progresses, the related tuft regions turn into sclerosis. In the present model FGS develops exclusively in areas of tuft adhesion.
在之前的一项研究[1]中,我们发现幼年大鼠进行单侧肾切除术后六个月内,残余肾脏中的肾小球会经历一系列严重变化,最终导致局灶节段性肾小球硬化(FGS)。已表明异常形状的毛细血管通道的形成是由局部系膜功能衰竭导致的,并且被认为是更严重病变发展的病灶。在本文中,我们描述并分析了足细胞结构中特征性病变的发展过程。与单侧肾切除术后肾小球的整体生长相伴,观察到足细胞明显肥大,而每个肾小球的足细胞平均数量并未改变。似乎足细胞无法维持与整个肾小球毛细血管丛相同程度的生长;足细胞肥大很快就会伴随适应性不良变化,最终导致细胞破坏。可以推测出以下病理变化顺序:细胞体在体积和面积上增大,同时细胞质片层显著变薄。初级突起变细并经常延伸至远处的毛细血管。总体而言,单个足细胞所服务的毛细血管面积显著增大。此外,扩张的细胞质片层(源自足细胞体)覆盖了毛细血管外表面(即滤过区域)越来越大的比例。因此,越来越多的滤液被输送到细胞体下间隙。这种滤液向尿腔流出受阻会导致覆盖其上的细胞质片层膨出形成假囊肿。覆盖在异常形状和扩张的毛细血管通道上的足细胞通常受影响最严重。肾小球毛细血管丛肥大、假囊肿形成和局部毛细血管扩张导致足细胞与鲍曼囊广泛贴附。贴附是肾小球毛细血管丛粘连发展的前提条件。在这些区域,足细胞从肾小球基底膜局部脱离,使得壁层细胞能够接触到肾小球基底膜。在早期粘连中,肾小球毛细血管丛与鲍曼囊的连接是由单个壁层细胞建立的,这些细胞同时附着于肾小球基底膜和鲍曼囊的基底膜。粘连被认为是节段性硬化的病灶;随着粘连进展,相关的肾小球毛细血管丛区域会变成硬化区域。在当前模型中,FGS仅在肾小球毛细血管丛粘连区域发展。
