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Serum Proteomic Signature of Human Chagasic Patients for the Identification of Novel Potential Protein Biomarkers of Disease

机译:查加斯人患者的血清蛋白质组学特征用于鉴定疾病的新型潜在蛋白质生物标志物

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摘要

Chagas disease is initiated upon infection by Trypanosoma cruzi. Among the health consequences is a decline in heart function, and the pathophysiological mechanisms underlying this manifestation are not well understood. To explore the possible mechanisms, we employed IgY LC10 affinity chromatography in conjunction with ProteomeLab PF2D and two-dimensional gel electrophoresis to resolve the proteome signature of high and low abundance serum proteins in chagasic patients. MALDI-TOF MS/MS analysis yielded 80 and 14 differentially expressed proteins associated with cardiomyopathy of chagasic and other etiologies, respectively. The extent of oxidative stress-induced carbonyl modifications of the differentially expressed proteins (n = 26) was increased and coupled with a depression of antioxidant proteins. Functional annotation of the top networks developed by ingenuity pathway analysis of proteome database identified dysregulation of inflammation/acute phase response signaling and lipid metabolism relevant to production of prostaglandins and arachidonic acid in chagasic patients. Overlay of the major networks identified prothrombin and plasminogen at a nodal position with connectivity to proteome signature indicative of heart disease (i.e., thrombosis, angiogenesis, vasodilatation of blood vessels or the aorta, and increased permeability of blood vessel and endothelial tubes), and inflammatory responses (e.g., platelet aggregation, complement activation, and phagocyte activation and migration). The detection of cardiac proteins (myosin light chain 2 and myosin heavy chain 11) and increased levels of vinculin and plasminogen provided a comprehensive set of biomarkers of cardiac muscle injury and development of clinical Chagas disease in human patients. These results provide an impetus for biomarker validation in large cohorts of clinically characterized chagasic patients.
机译:恰加斯氏锥虫感染后会引发南美锥虫病。在健康方面的后果包括心脏功能下降,并且对该表现基础的病理生理机制还没有很好的了解。为了探讨可能的机制,我们将IgY LC10亲和色谱法与ProteomeLab PF2D结合使用,并进行了二维凝胶电泳,以解决在甲壳类患者中高和低丰度血清蛋白的蛋白质组特征。 MALDI-TOF MS / MS分析分别产生了80种和14种差异表达的蛋白,分别与恰卡斯病和其他病因引起的心肌病相关。氧化应激诱导的差异表达蛋白的羰基修饰的程度(n = 26)增加,并伴有抗氧化蛋白的降低。通过蛋白质组数据库的机敏性路径分析开发的顶级网络功能注释,确定了与chagasic患者中与前列腺素和花生四烯酸产生有关的炎症/急性期反应信号传导和脂质代谢失调。主要网络的重叠在节点位置确定了凝血酶原和纤溶酶原,并与表明心脏病(即血栓形成,血管生成,血管或主动脉血管舒张以及血管和内皮管通透性增加)的蛋白质组特征具有连通性反应(例如血小板聚集,补体激活以及吞噬细胞激活和迁移)。心脏蛋白(肌球蛋白轻链2和肌球蛋白重链11)的检测,以及长春亭和纤溶酶原水平的提高,为人类患者的心肌损伤和临床Chagas疾病的发展提供了一整套综合的生物标记。这些结果为在临床上有特征的chagasic患者的大型队列中生物标志物验证提供了动力。

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