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首页> 外文期刊>Clinical chemistry and laboratory medicine: CCLM >Optimization and evaluation of surface-enhanced laser desorption/ionization time-of-flight mass spectrometry (SELDI-TOF MS) with reversed-phase protein arrays for protein profiling.
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Optimization and evaluation of surface-enhanced laser desorption/ionization time-of-flight mass spectrometry (SELDI-TOF MS) with reversed-phase protein arrays for protein profiling.

机译:使用反相蛋白质阵列进行蛋白质谱分析的表面增强激光解吸/电离飞行时间质谱(SELDI-TOF MS)的优化和评估。

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Surface-enhanced laser desorption/ionization (SELDI) time-of-flight mass spectrometry with protein arrays has facilitated the discovery of disease-specific protein profiles in serum. Such results raise hopes that protein profiles may become a powerful diagnostic tool. To this end, reliable and reproducible protein profiles need to be generated from many samples, accurate mass peak heights are necessary, and the experimental variation of the profiles must be known. We adapted the entire processing of protein arrays to a robotics system, thus improving the intra-assay coefficients of variation (CVs) from 45.1% to 27.8% (p<0.001). In addition, we assessed up to 16 technical replicates, and demonstrated that analysis of 2-4 replicates significantly increases the reliability of the protein profiles. A recent report on limited long-term reproducibility seemed to concord with our initial inter-assay CVs, which varied widely and reached up to 56.7%. However, we discovered that the inter-assay CV is strongly dependent on the drying time before application of the matrix molecule. Therefore, we devised a standardized drying process and demonstrated that our optimized SELDI procedure generates reliable and long-term reproducible protein profiles with CVs ranging from 25.7% to 32.6%, depending on the signal-to-noise ratio threshold used.
机译:具有蛋白质阵列的表面增强激光解吸/电离(SELDI)飞行时间质谱技术促进了血清中疾病特异性蛋白质谱的发现。这样的结果提出了希望,蛋白质谱可能会成为强大的诊断工具。为此,需要从许多样品中生成可靠且可重现的蛋白质图谱,准确的质量峰高是必需的,并且必须知道这些图谱的实验变化。我们将蛋白质阵列的整个处理过程调整为一个机器人系统,从而将测定内变异系数(CVs)从45.1%提高至27.8%(p <0.001)。此外,我们评估了多达16个技术重复,并证明对2-4个重复的分析显着提高了蛋白质谱的可靠性。最近关于长期可重复性有限的报告似乎与我们最初的测定间CV相符,其变异范围很大,最高可达56.7%。但是,我们发现测定间的CV强烈依赖于施加基质分子之前的干燥时间。因此,我们设计了标准化的干燥过程,并证明了我们优化的SELDI程序可生成可靠且可长期重现的蛋白质谱,其CV范围为25.7%至32.6%,具体取决于所使用的信噪比阈值。

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