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Broad-spectrum four-dimensional orthogonal electrophoresis: A novel comprehensively feasible system for protein complexomics investigation

机译:广谱四维正交电泳:一种新型的可行的蛋白质复合物组学研究系统

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摘要

The major challenge of "protein complexomics" is to separate intact protein complexes or interactional proteins without dissociation or denaturation from complex biological samples and to characterize structural subunits of protein complexes. To address these issues, we developed a novel approach termed "broad-spectrum four-dimensional orthogonal electrophoresis (BS4-DE) system," which is composed of a nondenaturing part I and denaturing part II. Here we developed a mild acidic-native-PAGE to constitute part I, together with native-thin-layer-IEF and basic-native-PAGE, widening the range of BS4-DE system application for extremely basic proteins with the range of pI from about 8 to 11 (there are obviously 1000 kinds of proteins in this interval), and also speculated on the mechanism of separating. We first proposed ammonium hydroxide-ultrasonic protein extractive strategy as a seamless connection between part I and part II, and also speculated on the extractive mechanism. More than 4000 protein complexes could be theoretically solved by this system. Using this approach, we focus on blood rich in protein complexes which make it challenging to sera/ plasma proteome study. Our results indicated that the BS4-DE system could be applied to blood protein complexomics investigation, providing a comprehensively feasible approach for disease proteomics.
机译:“蛋白质复合物组学”的主要挑战是从完整的生物样品中分离完整的蛋白质复合物或相互作用的蛋白质而不发生解离或变性,并表征蛋白质复合物的结构亚基。为了解决这些问题,我们开发了一种新颖的方法,称为“广谱四维正交电泳(BS4-DE)系统”,它由非变性部分I和变性部分II组成。在这里,我们开发了一种温和的酸性-天然-PAGE,与天然薄层-IEF和碱性-天然-PAGE一起构成了第I部分,扩大了BS4-DE系统在pI范围从大约有8到11种(在此间隔中显然有1000种蛋白质),并且还推测了其分离机理。我们首先提出了氢氧化铵-超声波蛋白质的提取策略,作为第一部分和第二部分之间的无缝连接,并推测了其提取机理。该系统理论上可以解决4000多种蛋白质复合物。使用这种方法,我们专注于富含蛋白质复合物的血液,这使其难以进行血清/血浆蛋白质组学研究。我们的结果表明,BS4-DE系统可用于血液蛋白复合物研究,为疾病蛋白质组学提供了一种全面可行的方法。

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