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首页> 外文期刊>Proteomics >A Combination of Proteomic Approaches Identifies A Panel of Circulating Extracellular Vesicle Proteins Related to the Risk of Suffering Cardiovascular Disease in Obese Patients
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A Combination of Proteomic Approaches Identifies A Panel of Circulating Extracellular Vesicle Proteins Related to the Risk of Suffering Cardiovascular Disease in Obese Patients

机译:蛋白质组学方法的组合鉴定了与肥胖患者患心血管疾病的风险有关的循环细胞外囊泡蛋白的面板

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Plasma-derived extracellular vesicles (EVs) have been extensively described as putative biomarkers in different diseases. Interestingly, increased levels of EVs subpopulations are well known to associate with obesity. The goal of this study is to identify EVs-derived biomarkers in plasma from obese patients in order to predict the development of pathological events associated with obesity. Samples are obtained from 22 obese patients and their lean-matched controls are divided into two cohorts: one for a 2D fluorescence difference gel electrophoresis (2D-DIGE)-based study, and the other one for a label free LC-MS/MS-based approach. EVs are isolated following a serial ultracentrifugation protocol. Twenty-two and 23 differentially regulated features are detected from 2D-DIGE and label free LC-MS/MS, respectively; most of them involve in the coagulation and complement cascades. Remarkably, there is an upregulation of complement C4, complement C3, and fibrinogen in obese patients following both approaches, the latter two also validated by 2D-western-blotting in an independent cohort. These results correlate with a proinflammatory and prothrombotic state of those individuals. On the other hand, a downregulation of adiponectin leading to an increased risk of suffering cardiovascular diseases has been shown. The results suggest the relevance of plasma-derived-EVs proteins as a source of potential biomarkers for the development of atherothrombotic events in obesity.
机译:等离子体衍生的细胞外囊泡(EVS)已被广泛地描述为不同疾病的推定生物标志物。有趣的是,众所周知,EVS群体的增加程度是富有肥胖症的。本研究的目标是从肥胖患者中鉴定血浆中的EVS衍生的生物标志物,以预测与肥胖症相关的病理事件的发展。从22例肥胖的患者获得样品,将它们的瘦匹配对照分为两个队列:一个用于2D荧光差异凝胶电泳(2D-Dige)的研究,另一个用于标签LC-MS / MS-基于方法。串行超速离心协议后,EVS被隔离。从2D-Dige检测到二十二和23个差异调节的特征,分别检测到免费LC-MS / MS;其中大多数涉及凝血和补充瀑布。值得注意的是,在两种方法后,肥胖患者的补体C4,补体C3和纤维蛋白原有一个上调,后两者也通过独立队列中的2D-Western-Blotting验证。这些结果与这些个体的促炎和癌细胞状况相关。另一方面,已经显示出脂联素的下调导致患有心血管疾病的风险增加。结果表明,血浆衍生EVS蛋白作为肥胖症中动脉萎缩事件的潜在生物标志物的来源的相关性。

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