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首页> 外文期刊>Journal of proteome research >Prediction of an Upper Limit for the Fraction of Interprotein Cross-Links in Large-Scale In Vivo Cross-Linking Studies
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Prediction of an Upper Limit for the Fraction of Interprotein Cross-Links in Large-Scale In Vivo Cross-Linking Studies

机译:在体内交联研究中大规模诠释蛋白交叉链路分数的上限预测

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摘要

Chemical cross-linking and mass spectrometry is of growing use for establishment of distance constraints on protein conformations and interactions. Whereas intraprotein cross-links can arise from proteins in isolation, interprotein cross-links reflect proximity of two interacting proteins in the sample. Prediction of expected ratios of the number of interprotein to intraprotein cross-links is hindered by lacking comprehensive knowledge on the interactome network and global occupancy levels for all interacting complex subunits. Here we determine the theoretical number of possible inter-and intraprotein cross-links in available PDB structures of proteins bound in complexes to predict a maximum expected fraction of interprotein cross-links in large scale in vivo cross-linking studies. We show how the maximum fraction can guide interpretation of reported interprotein fractions with respect to the extent of sample protein binding, comparing whole cell and lysate cross-linked samples as an example. We also demonstrate how an observation of interprotein cross-link fractions greater than the maximum value can result from the presence of false positive cross-links which are predominantly interprotein, their number estimable from the observed surplus fraction of interprotein cross-links.
机译:化学交联和质谱越来越多地用于建立蛋白质构象和相互作用的距离约束。虽然Introaprotein交联可以从蛋白质中分离出现,但是诠释十字链路反映了样品中两个相互作用蛋白的接近。通过缺乏关于所有互动复合亚基的互乱网络和全球占用水平的全面知识,阻碍了对脑内蛋白交联蛋白交联的预期比率的预测。在这里,我们确定可用的蛋白质的可用PDB结构中可能的蛋白质和肠球状蛋白交联的理论数量,以预测大规模在体内交联研究中大规模的最大预期分数。我们展示了最大馏分如何指导报告的诠释术语关于样品蛋白结合的程度,比较全细胞和裂解物交联样品作为一个例子。我们还证明了如何观察大于最大值的译文的交联级分的观察可能是由于主要展示蛋白的假阳性交联的存在导致它们的数量从观察到的译文交叉链路的差异分数估计。

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