Hur Oscar, Karplus Kevin
PO Box 2548, Sunnyvale, CA 94087-0548 and Department of Biomolecular Engineering, University of California at Santa Cruz, Santa Cruz, CA 95064. USA.
Protein Eng Des Sel. 2005 Dec;18(12):597-605. doi: 10.1093/protein/gzi068. Epub 2005 Oct 24.
This paper proposes a strategy to translate experimental 1H NMR proton distance restraints into their corresponding heavy atom distance restraints for the purpose of protein structure prediction. The relationships between interproton distances and the corresponding heavy atom distances are determined by studying well-resolved X-ray protein structures. The data from the interproton distances of amide protons, alpha-protons, beta-protons and side chain methyl protons are plotted against the corresponding heavy atoms in scatter plots and then fitted with linear equations for lower bounds, upper bounds and optimal fits. We also transform the scatter plots into two-dimensional heat maps and three-dimensional histograms, which identify the regions where data points concentrate. The common interproton distances between amide protons, alpha-protons, beta-protons in alpha-helices, anti-parallel beta-sheets and parallel beta-sheets are also tabulated. We have found several patterns emerging from the distance relationships between heavy atom pairs and their corresponding proton pairs. All our upper bound, lower bound and optimal fit results for translating the interproton distance into their corresponding heavy atom distances are tabulated.
本文提出了一种策略,用于将实验性的1H NMR质子距离约束转换为相应的重原子距离约束,以用于蛋白质结构预测。通过研究解析良好的X射线蛋白质结构,确定质子间距离与相应重原子距离之间的关系。将酰胺质子、α-质子、β-质子和侧链甲基质子的质子间距离数据与相应的重原子绘制在散点图中,然后用线性方程拟合下限、上限和最佳拟合。我们还将散点图转换为二维热图和三维直方图,以识别数据点集中的区域。还列出了α-螺旋、反平行β-折叠和平行β-折叠中酰胺质子、α-质子、β-质子之间常见的质子间距离。我们发现了重原子对与其相应质子对之间距离关系中出现的几种模式。我们将质子间距离转换为相应重原子距离的所有上限、下限和最佳拟合结果都列成了表格。