Urine proteome profile in primary podocytopathies

A. Vinogradov, N. Chebotareva, A. Bugrova, A. G. Brzhozovskij, T. Krasnova, S. Moiseev, A. Kononikhin
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Abstract

   BACKGROUND. Primary focal segmental glomerulosclerosis (FSGS) and membranous nephropathy (MN) are diseases with primary podocyte damage with high proteinuria and nephrotic syndrome. While the mechanisms in primary MN are well understood, the pathogenesis of primary FSGS is still unknown, and therefore, the search for biomarkers that could expand ourunderstanding of its pathogenetic mechanisms.   THE AIM: to determine the urine proteomic profile of patients with primary podocytopathies – FSGS in comparison with MN.   PATIENTS AND METHODS. The study included 48 patients with a morphologically confirmed diagnosis of CGN occurring with nephrotic syndrome – 32 men and 16 women. In 18 patients, a decrease in glomerular filtration rate < 60 ml/min/1.73 m2 was observed. The histological diagnosis was confirmed by biopsy: 31 patients had FSGS, 17 patients with MN were included as a comparison group. The study of the urinary proteome was carried out by high performance liquid chromatography/mass spectrometry. RESULTS. In patients with FSGS, compared with the MN group, an increased content of 22 different proteins was noted, the most abundant were apolipoprotein A-I, hemopexin, vitronectin, pigment epithelial growth factor, components of the complement system (C3, C4b, factors B and H), retinol – and vitamin D-binding proteins, alpha-2-HS-glycoprotein, histidine-rich glycoprotein, plasma C1 protease inhibitor. In MN, increased urinary excretion of the complement component C2, fibrinogen alpha chain, osteopontin, and the SH3 domain-binding glutamic acid-rich-like protein 3, was detected.   CONCLUSION. The proteomic profile of urine in FSGS, compared to MN, reflects the activation of variety of pathological processes – podocyte damage, involvement of parietal epithelial cells, tubulo-interstitial damage, accumulation of extracellular matrix, and complement activation process.
原发性足细胞病的尿蛋白质组谱
背景。原发性局灶节段性肾小球硬化(FSGS)和膜性肾病(MN)是原发性足细胞损伤伴高蛋白尿和肾病综合征的疾病。虽然原发性MN的机制已经被很好地理解,但原发性FSGS的发病机制仍然未知,因此,寻找生物标志物可以扩大我们对其发病机制的理解。目的:确定原发性足细胞病变(FSGS)患者的尿液蛋白质组学特征,并与MN进行比较。患者和方法。该研究包括48例形态学确诊为肾病综合征的CGN患者,其中32名男性,16名女性。18例患者肾小球滤过率< 60 ml/min/1.73 m2。活检证实组织学诊断:31例FSGS患者,17例MN患者作为对照组。采用高效液相色谱/质谱法对尿蛋白组进行研究。结果。在FSGS患者中,与MN组相比,22种不同蛋白的含量增加,其中最丰富的是载脂蛋白A-I、血凝素、玻璃体粘连素、色素上皮生长因子、补体系统成分(C3、C4b、因子B和H)、视黄醇和维生素d结合蛋白、α -2- hs糖蛋白、富组氨酸糖蛋白、血浆C1蛋白酶抑制剂。在MN中,检测到补体成分C2、纤维蛋白原α链、骨桥蛋白和SH3结构域结合谷氨酸样蛋白3的尿排泄增加。结论。与MN相比,FSGS患者尿液的蛋白质组学特征反映了多种病理过程的激活——足细胞损伤、壁上皮细胞受累、小管间质损伤、细胞外基质积累和补体激活过程。
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