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Proteomics analysis of human coronary atherosclerotic plaque: a feasibility study of direct tissue proteomics by liquid chromatography and tandem mass spectrometry.

机译:人类冠状动脉粥样斑块的蛋白质组学分析:通过液相色谱和串联质谱法对直接组织蛋白质组学进行可行性研究。

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摘要

Cardiovascular disease presents significant variations in human populations with respect to the atherosclerotic plaque progression, inflammation, thrombosis, and rupture. To gain a more comprehensive picture of the pathogenic mechanism of atherosclerosis and the variations seen in patients, efficient methods to identify proteins from the normal and diseased arteries need to be developed. To accomplish this goal, we tested the feasibility and efficiency of protein identification by a recently developed method, termed direct tissue proteomics (DTP). We analyzed frozen and paraformaldehyde-fixed archival coronary arteries with the DTP method. We also validated the distinct expression of four proteins by immunohistochemistry. In addition, we demonstrated the compatibility of the DTP method with laser capture microdissection and the possibility of monitoring specific cytokines and growth factors by the absolute quantification of abundance method. Major findings from this feasibility study are that 1) DTP can be used to efficiently identify proteins from paraformaldehyde-fixed, paraffin-embedded, and frozen coronary arteries; 2) approximately twice the number of proteins were identified from the frozen sections when compared with the paraformaldehyde-fixed sections; 3) laser capture microdissection is compatible with DTP; and 4) detection of low abundance cytokines and growth factors in the coronary arteries required selective reaction monitoring experiments coupled to absolute quantification of abundance. The analysis of 35 human coronary atherosclerotic samples allowed identification of a total of 806 proteins. The present study provides the first large scale proteomics map of human coronary atherosclerotic plaques.
机译:在动脉粥样硬化斑块进展,炎症,血栓形成和破裂方面,心血管疾病在人群中呈现出显着差异。为了更全面地了解动脉粥样硬化的致病机制及其在患者中所见的变异,需要开发一种从正常和患病动脉中鉴定蛋白质的有效方法。为实现此目标,我们通过一种称为直接组织蛋白质组学(DTP)的最新开发方法测试了蛋白质鉴定的可行性和效率。我们用DTP方法分析了冷冻和低聚甲醛固定的档案冠状动脉。我们还通过免疫组织化学验证了四种蛋白质的独特表达。此外,我们证明了DTP方法与激光捕获显微切割法的兼容性以及通过绝对定量方法定量监测特定细胞因子和生长因子的可能性。这项可行性研究的主要发现是:1)DTP可用于从多聚甲醛固定,石蜡包埋和冷冻的冠状动脉中有效鉴定蛋白质; 2)与多聚甲醛固定的切片相比,从冷冻切片中鉴定出的蛋白质数量大约是两倍; 3)激光捕获显微切割与DTP兼容;和4)在冠状动脉中检测低丰度细胞因子和生长因子需要选择性的反应监测实验,以及丰度的绝对定量。对35例人类冠状动脉粥样硬化样品的分析可以鉴定总共806种蛋白质。本研究提供了人类冠状动脉粥样斑块的第一个大规模蛋白质组图。

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