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Solvent interaction analysis as a proteomic approach to structure-based biomarker discovery and clinical diagnostics

机译:溶剂相互作用分析作为蛋白质组学方法,用于基于结构的生物标志物发现和临床诊断

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摘要

Proteins have several measurable features in biological fluids that may change under pathological conditions. The current disease biomarker discovery is mostly based on protein concentration in the sample as the measurable feature. Changes in protein structures, such as post-translational modifications and in protein-partner interactions are known to accompany pathological processes. Changes in glycosylation profiles are well-established for many plasma proteins in various types of cancer and other diseases. The solvent interaction analysis method is based on protein partitioning in aqueous two-phase systems and is highly sensitive to changes in protein structure and protein-protein- and protein-partner interactions while independent of the protein concentration in the biological sample. It provides quantitative index: partition coefficient representing changes in protein structure and interactions with partners. The fundamentals of the method are presented with multiple examples of applications of the method to discover and monitor structural protein biomarkers as disease-specific diagnostic indicators.
机译:蛋白质在生物体液中具有几种可测量的特征,这些特征可能会在病理条件下发生变化。当前疾病生物标志物的发现主要基于样品中蛋白质的浓度作为可测量的特征。已知蛋白质结构的变化,例如翻译后修饰和蛋白质-伴侣相互作用,伴随着病理过程。对于各种类型的癌症和其他疾病中的许多血浆蛋白,糖基化谱的变化是公认的。溶剂相互作用分析方法基于水两相系统中的蛋白质分配,并且对蛋白质结构的变化以及蛋白质-蛋白质和蛋白质-伴侣相互作用的变化高度敏感,而与生物样品中蛋白质的浓度无关。它提供了定量指标:分配系数,代表蛋白质结构的变化以及与伴侣的相互作用。介绍了该方法的基本原理,并列举了该方法的许多应用实例,以发现和监测作为疾病特异性诊断指标的结构蛋白生物标志物。

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