Zeisberg Michael, Khurana Mona, Rao Velidi H, Cosgrove Dominic, Rougier Jean-Philippe, Werner Michelle C, Shield Charles F, Werb Zena, Kalluri Raghu
Center for Matrix Biology, Department of Medicine, Beth Israel Deaconess Medical Center and Harvard Medical School, Boston, Massachusetts, USA.
PLoS Med. 2006 Apr;3(4):e100. doi: 10.1371/journal.pmed.0030100. Epub 2006 Mar 7.
Glomerular basement membrane (GBM), a key component of the blood-filtration apparatus in the in the kidney, is formed through assembly of type IV collagen with laminins, nidogen, and sulfated proteoglycans. Mutations or deletions involving alpha3(IV), alpha4(IV), or alpha5(IV) chains of type IV collagen in the GBM have been identified as the cause for Alport syndrome in humans, a progressive hereditary kidney disease associated with deafness. The pathological mechanisms by which such mutations lead to eventual kidney failure are not completely understood.
We showed that increased susceptibility of defective human Alport GBM to proteolytic degradation is mediated by three different matrix metalloproteinases (MMPs)--MMP-2, MMP-3, and MMP-9--which influence the progression of renal dysfunction in alpha3(IV)-/- mice, a model for human Alport syndrome. Genetic ablation of either MMP-2 or MMP-9, or both MMP-2 and MMP-9, led to compensatory up-regulation of other MMPs in the kidney glomerulus. Pharmacological ablation of enzymatic activity associated with multiple GBM-degrading MMPs, before the onset of proteinuria or GBM structural defects in the alpha3(IV)-/- mice, led to significant attenuation in disease progression associated with delayed proteinuria and marked extension in survival. In contrast, inhibition of MMPs after induction of proteinuria led to acceleration of disease associated with extensive interstitial fibrosis and early death of alpha3(IV)-/- mice.
These results suggest that preserving GBM/extracellular matrix integrity before the onset of proteinuria leads to significant disease protection, but if this window of opportunity is lost, MMP-inhibition at the later stages of Alport disease leads to accelerated glomerular and interstitial fibrosis. Our findings identify a crucial dual role for MMPs in the progression of Alport disease in alpha3(IV)-/- mice, with an early pathogenic function and a later protective action. Hence, we propose possible use of MMP-inhibitors as disease-preventive drugs for patients with Alport syndrome with identified genetic defects, before the onset of proteinuria.
肾小球基底膜(GBM)是肾脏血液滤过装置的关键组成部分,由IV型胶原蛋白与层粘连蛋白、巢蛋白和硫酸化蛋白聚糖组装而成。已确定GBM中涉及IV型胶原蛋白的α3(IV)、α4(IV)或α5(IV)链的突变或缺失是人类奥尔波特综合征的病因,这是一种与耳聋相关的进行性遗传性肾脏疾病。此类突变导致最终肾衰竭的病理机制尚未完全明确。
我们发现,缺陷型人类奥尔波特GBM对蛋白水解降解的易感性增加是由三种不同的基质金属蛋白酶(MMP)——MMP-2、MMP-3和MMP-9介导的,它们影响α3(IV)-/-小鼠(一种人类奥尔波特综合征模型)肾功能障碍的进展。MMP-2或MMP-9的基因敲除,或MMP-2和MMP-9两者的基因敲除,导致肾小球中其他MMP的代偿性上调。在α3(IV)-/-小鼠出现蛋白尿或GBM结构缺陷之前,对与多种降解GBM的MMP相关的酶活性进行药物性抑制,导致疾病进展显著减轻,蛋白尿延迟出现,生存期显著延长。相比之下,在蛋白尿诱导后抑制MMP会导致疾病加速发展,伴有广泛的间质纤维化和α3(IV)-/-小鼠早期死亡。
这些结果表明,在蛋白尿出现之前保持GBM/细胞外基质的完整性可显著保护疾病,但如果失去这个机会窗口,在奥尔波特病后期抑制MMP会导致肾小球和间质纤维化加速。我们的研究结果确定了MMP在α3(IV)-/-小鼠奥尔波特病进展中的关键双重作用,具有早期致病功能和后期保护作用。因此,我们建议在蛋白尿出现之前,对于已确定基因缺陷的奥尔波特综合征患者,可能使用MMP抑制剂作为疾病预防药物。
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