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Characterization of the renal cyst fluid proteome in autosomal dominant polycystic kidney disease (ADPKD) patients

机译:常染色体显性遗传性多囊肾病(ADPKD)患者肾囊液蛋白质组的表征

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摘要

Autosomal dominant polycystic kidney disease (ADPKD) is characterized by localized autonomous cellular proliferation, fluid accumulation within the cysts, and intraparenchymal fibrosis of the kidney. Little is known about the cyst fluid's protein composition. We hypothesized that the complex collection of cyst fluid proteins (cyst fluid proteome) plays a major role in cyst formation/maintenance and contains yet unknown diagnostic and mechanistic features that are common to all forms of PKD. We analyzed five kidney cyst fluids from four patients with ADPKD. Tryptic peptides from plasma-protein immunodepleted (ProteoPrep®) and undepleted cyst fluid samples were analyzed by LC-MS/MS. Proteins were identified by SEQUEST™ and validated via the Trans-Proteomic Pipeline; 391 proteins were identified with >90% confidence; 251 of them in undepleted and 362 in immunodepleted samples. Immunodepletion removed >94% of the cyst fluid protein. A surprisingly large and functionally diverse number of proteins common to most cysts were identified. These proteins may be of mechanistic interest and include Ig γ, κ, and fragments; complement components; vitronectin; orosomucoid; prostaglandin D2 synthase; vitamin D-binding protein; clusterin; SERPIN family proteins; hemopexin; and fetuin-A. Additionally, these results suggest that further prefractionation and enhanced chromatographic separation of tryptic peptides is likely to expose an even greater number of relevant proteins.
机译:常染色体显性遗传性多囊肾病(ADPKD)的特征是局部自主性细胞增殖,囊肿内积液和肾脏实质内纤维化。关于囊液的蛋白质组成知之甚少。我们假设复杂的囊液蛋白(囊液蛋白质组)集合在囊肿的形成/维持中起着重要作用,并且还包含所有形式的PKD所共有的未知的诊断和机制特征。我们分析了四名ADPKD患者的五种肾囊肿液。通过LC-MS / MS分析了血浆蛋白免疫缺陷(ProteoPrep®)和未耗尽的囊液样品中的胰蛋白酶肽。通过SEQUEST™鉴定蛋白质,并通过跨蛋白质组学管道进行验证;鉴定出391种蛋白质,> 90%的置信度;其中251份未消耗样品和362份未消耗免疫样品。免疫清除去除了> 94%的囊液蛋白。鉴定出了大多数囊肿共有的数量惊人且数量众多的蛋白质。这些蛋白质可能具有机械作用,包括Igγ,κ和片段。补体成分;玻璃连蛋白类骨胶前列腺素D2合酶;维生素D结合蛋白;簇蛋白SERPIN家族蛋白;血色素和胎球蛋白-A。此外,这些结果表明,胰蛋白酶肽的进一步预分离和增强的色谱分离可能会暴露更多的相关蛋白质。

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