Glomerular Disease Therapeutics Laboratory, University of Alabama at Birmingham, USA.
Am J Kidney Dis. 2012 Feb;59(2):284-92. doi: 10.1053/j.ajkd.2011.07.024. Epub 2011 Oct 5.
The pathogenesis of minimal change disease (MCD), considered to be the simplest form of nephrotic syndrome, has been one of the major unsolved mysteries in kidney disease. In this review, recent landmark studies that have led to the unraveling of MCD are discussed. A recent study now explains the molecular basis of major clinical and morphologic changes in MCD. Overproduction of angiopoietin-like 4 (ANGPTL4) in podocytes in MCD causes binding of ANGPTL4 to the glomerular basement membrane, development of nephrotic-range selective proteinuria, diffuse effacement of foot processes, and loss of glomerular basement membrane charge, but is not associated with changes shown by light microscopy in the glomerular and tubulointerstitial compartments. At least some of this ability of ANGPTL4 to induce proteinuria is linked to a deficiency of sialic acid residues because oral supplementation with sialic acid precursor N-acetyl-d-mannosamine improves sialylation of podocyte-secreted ANGPTL4 and significantly decreases proteinuria. Animal models of MCD, recent advances in potential biomarkers, and studies of upstream factors that may initiate glomerular changes also are discussed. In summary, recent progress in understanding MCD is likely to influence the diagnosis and treatment of MCD in the near future.
微小病变病(MCD)的发病机制一直是肾脏疾病中未解决的主要难题之一,被认为是肾病综合征中最简单的形式。在这篇综述中,讨论了最近导致 MCD 阐明的具有里程碑意义的研究。最近的一项研究现在解释了 MCD 中主要临床和形态学变化的分子基础。MCD 足细胞中血管生成素样蛋白 4(ANGPTL4)的过度产生导致 ANGPTL4 与肾小球基底膜结合,出现肾病范围的选择性蛋白尿、足突弥漫性消失和肾小球基底膜电荷丧失,但与肾小球和肾小管间质腔中光镜下显示的变化无关。ANGPTL4 诱导蛋白尿的这种能力至少部分与唾液酸残基缺乏有关,因为口服唾液酸前体 N-乙酰-D-甘露糖胺可以改善足细胞分泌的 ANGPTL4 的唾液酸化,并显著减少蛋白尿。还讨论了 MCD 的动物模型、潜在生物标志物的最新进展以及可能引发肾小球变化的上游因素的研究。总之,对 MCD 的理解的最新进展可能会在不久的将来影响 MCD 的诊断和治疗。