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Replacing immunoassays with tryptic digestion-peptide immunoaffinity enrichment and LC-MS/MS

机译:用胰蛋白酶消化肽免疫亲和富集和LC-MS / MS代替免疫测定

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摘要

For decades, immunoassays have provided the framework for protein biomarker studies in clinical medicine and in therapeutic monitoring for drug development. At the same time, investigators have uncovered many issues that make immunoassays unreliable in many human serum and plasma samples. LC-MS/MS after tryptic digestion of proteins is potentially an attractive solution, but the sensitivity of the method is not sufficient to measure many important low-abundance proteins directly. The use of antipeptide antibodies to immunoenrich peptides of interest can improve the sensitivity of the approach, greatly simplify the matrix enabling shortened chromatographic runs, and facilitate the multiplexed quantification of analytes, which could reduce the costs of quantitative protein measurements in complex specimens. We provide an overview of the method and the steps needed to develop an assay. In addition, we review the efforts to make this method generally more applicable.
机译:数十年来,免疫分析为临床医学和药物开发的治疗性监测中的蛋白质生物标志物研究提供了框架。同时,研究人员发现了许多问题,这些问题使免疫测定在许多人血清和血浆样品中不可靠。胰蛋白酶消化蛋白质后的LC-MS / MS可能是一种有吸引力的解决方案,但该方法的灵敏度不足以直接测量许多重要的低丰度蛋白质。使用针对感兴趣的免疫富集肽的抗肽抗体可以提高方法的灵敏度,大大简化基质,缩短色谱运行时间,并促进分析物的多重定量,这可以降低复杂样品中定量蛋白质测量的成本。我们提供了开发方法所需的方法和步骤的概述。此外,我们回顾了使该方法更普遍适用的工作。

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