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在尿液和肾结石患者结石基质中,经蛋白质组学方法鉴定到的炎症和纤维蛋白在蛋白质组层面被鉴定为关键蛋白成分。

Inflammatory and fibrotic proteins proteomically identified as key protein constituents in urine and stone matrix of patients with kidney calculi.

机构信息

Department of Biochemistry, Faculty of Medicine, Chulalongkorn University, Bangkok 10330 Thailand.

Department of Biochemistry, Faculty of Medicine, Chulalongkorn University, Bangkok 10330 Thailand.

出版信息

Clin Chim Acta. 2014 Feb 15;429:81-9. doi: 10.1016/j.cca.2013.11.036. Epub 2013 Dec 9.

Abstract

To uncover whether urinary proteins are incorporated into stones, the proteomic profiles of kidney stones and urine collected from the same patients have to be explored. We employed 1D-PAGE and nanoHPLC-ESI-MS/MS to analyze the proteomes of kidney stone matrix (n=16), nephrolithiatic urine (n=14) and healthy urine (n=3). We identified 62, 66 and 22 proteins in stone matrix, nephrolithiatic urine and healthy urine, respectively. Inflammation- and fibrosis-associated proteins were frequently detected in the stone matrix and nephrolithiatic urine. Eighteen proteins were exclusively found in the stone matrix and nephrolithiatic urine, considered as candidate biomarkers for kidney stone formation. S100A8 and fibronectin, representatives of inflammation and fibrosis, respectively, were up-regulated in nephrolithiasis renal tissues. S100A8 was strongly expressed in infiltrated leukocytes. Fibronectin was over-expressed in renal tubular cells. S100A8 and fibronectin were immunologically confirmed to exist in nephrolithiatic urine and stone matrix, but in healthy urine they were undetectable. Conclusion, both kidney stones and urine obtained from the same patients greatly contained inflammatory and fibrotic proteins. S100A8 and fibronectin were up-regulated in stone-baring kidneys and nephrolithiatic urine. Therefore, inflammation and fibrosis are suggested to be involved in the formation of kidney calculi.

摘要

为了揭示尿蛋白是否被纳入结石,必须探索来自同一患者的肾结石和尿液的蛋白质组学特征。我们采用 1D-PAGE 和纳升 HPLC-ESI-MS/MS 分析了肾结石基质(n=16)、肾结石患者尿液(n=14)和健康尿液(n=3)的蛋白质组。我们分别在结石基质、肾结石患者尿液和健康尿液中鉴定到 62、66 和 22 种蛋白质。在结石基质和肾结石患者尿液中频繁检测到与炎症和纤维化相关的蛋白质。有 18 种蛋白质仅存在于结石基质和肾结石患者尿液中,被认为是肾结石形成的候选生物标志物。S100A8 和纤维连接蛋白分别是炎症和纤维化的代表,在肾结石肾组织中上调。S100A8 在浸润的白细胞中强烈表达。纤维连接蛋白在肾小管细胞中过度表达。免疫组化法证实 S100A8 和纤维连接蛋白存在于肾结石患者尿液和结石基质中,但在健康尿液中无法检测到。结论:来自同一患者的肾结石和尿液均含有大量的炎症和纤维化蛋白。S100A8 和纤维连接蛋白在有结石的肾脏和肾结石患者尿液中上调。因此,炎症和纤维化可能参与了肾结石的形成。

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