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Urine proteomics of primary membranous nephropathy using nanoscale liquid chromatography tandem mass spectrometry analysis

机译:纳米级液相色谱串联质谱分析原发性膜性肾病的尿蛋白质组学

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Primary membranous nephropathy (PMN) is an important cause of nephrotic syndrome in adults. Urine proteome may provide important clues of pathophysiological mechanisms in PMN. In the current study, we analyzed and compared the proteome of urine from patients with PMN and normal controls. We performed two technical replicates (TMT1 and TMT2) to analyze and compare the urine proteome from patients with PMN and normal controls by tandem mass tag (TMT) technology coupled with nanoscale liquid chromatography tandem mass spectrometry analysis (LC–MS/MS). Gene ontology (GO) enrichment analysis was performed to analyse general characterization of the proteins. The proteins were also matched against the database of Kyoto Encyclopedia of Genes and Genomes (KEGG). For validation, Western blot was used to analyze the selected proteins. A total of 509 proteins and 411 proteins were identified in TMT1 and TMT2, respectively. 249 proteins were both identified in two technical replicates. GO analysis and KEGG analysis revealed immunization and coagulation were predominantly involved. Among the differential protein, the overexcretion of alpha-1-antitrypsin (A1AT) and afamin (AFM) were validated by Western blot analysis. Our data showed the important role of immunologic mechanism in the development of PMN, and the value of urinary A1AT and AFM in biomarker discovery of patients with PMN. The discovery of the overexcretion of A1AT and AFM in the urine can help to further elucidate pathogenetic mechanisms involved in PMN.
机译:原发性膜性肾病(PMN)是成人肾病综合征的重要原因。尿蛋白质组可能为PMN的病理生理机制提供重要线索。在本研究中,我们分析并比较了PMN患者和正常对照者尿液中的蛋白质组。我们进行了两个技术重复试验(TMT1和TMT2),以通过串联质谱标签(TMT)技术结合纳米级液相色谱串联质谱分析(LC-MS / MS)分析和比较PMN患者和正常对照患者的尿蛋白。进行基因本体论(GO)富集分析以分析蛋白质的一般特征。这些蛋白质还与《京都议定书基因与基因组百科全书》(KEGG)的数据库相匹配。为了验证,使用蛋白质印迹法分析所选的蛋白质。在TMT1和TMT2中分别鉴定出总共509个蛋白和411个蛋白。在两次技术重复中鉴定出249种蛋白质。 GO分析和KEGG分析显示主要涉及免疫和凝血。在差异蛋白中,通过蛋白质印迹分析验证了α-1-抗胰蛋白酶(A1AT)和afamin(AFM)的过度表达。我们的数据显示了免疫机制在PMN发育中的重要作用,以及尿A1AT和AFM在PMN患者生物标志物发现中的价值。尿液中A1AT和AFM过度分泌的发现可以帮助进一步阐明参与PMN的致病机制。

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