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The beginning of a beautiful friendship: Cross-linking/mass spectrometry and modelling of proteins and multi-protein complexes

机译:美好友谊的开始:蛋白质/多蛋白质复合物的交联/质谱分析和建模

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摘要

After more than a decade of method development, cross-linking in combination with mass spectrometry and bioinformatics is finally coming of age. This technology now provides improved opportunities for modelling by mapping structural details of functional complexes in solution. The structure of proteins or protein complexes is ascertained by identifying amino acid pairs that are positioned in close proximity to each other. The validity of this technique has recently been benchmarked for large multi-protein complexes, by comparing cross-link data with that from a crystal structure of RNA polymerase II. Here, the specific nature of this cross-linking data will be discussed to assess the technical challenges and opportunities for model building. We believe that once remaining technological challenges of cross-linking/mass spectrometry have been addressed and cross-linking/mass spectrometry data has been incorporated into modelling algorithms it will quickly become an indispensable companion of protein and protein complex modelling and a corner-stone of integrated structural biology.
机译:经过十多年的方法开发,结合​​质谱和生物信息学的交联终于成熟。通过映射解决方案中功能复合物的结构细节,该技术现在为建模提供了更多的机会。蛋白质或蛋白质复合物的结构是通过鉴定彼此紧邻的氨基酸对来确定的。通过将交联数据与RNA聚合酶II晶体结构的数据进行比较,最近将该技术的有效性作为大型多蛋白复合物的基准。在此,将讨论此交叉链接数据的特定性质,以评估技术挑战和建立模型的机会。我们相信,一旦解决了交联/质谱的其余技术难题,并将交联/质谱数据纳入了建模算法,它将迅速成为蛋白质和蛋白质复合物建模的必不可少的伴侣,并成为综合结构生物学。

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