Size‐independent comparison of protein three‐dimensional structures

切断 回转半径 数学 相似性(几何) 超球体 叠加原理 转动惯量 链条(单位) 安萨茨 物理 数学分析 几何学 统计物理学 经典力学 数学物理 量子力学 核磁共振 图像(数学) 人工智能 计算机科学 聚合物
作者
Vladimir N. Maiorov,Gordon M. Crippen
出处
期刊:Proteins [Wiley]
卷期号:22 (3): 273-283 被引量:140
标识
DOI:10.1002/prot.340220308
摘要

Abstract Protein structures are routinely compared by their root‐mean‐square deviation (RMSD) in atomic coordinates after optimal rigid body superposition. What is not so clear is the significance of different RMSD values, particularly above the customary arbitrary cutoff for obvious similarity of 2–3 Å. Our earlier work argued for an intrinsic cutoff for protein similarity that varied with the number of residues in the polypeptide chains being compared. Here we introduce a new measure, ρ, of structural similarity based on RMSD that is independent of the sizes of the molecules involved, or of any other special properties of molecules. When ρ is less than 0.4–0.5, protein structures are visually recognized to be obviously similar, but the mathematically pleasing intrinsic cutoff of ρ>1.0 corresponds to overall similarity in folding motif at a level not usually recognized until smoothing of the polypeptide chain path makes it striking. When the structures are scaled to unit radius of gyration and equal principle moments of inertia, the comparisons are even more universal, since they are no longer obscured by differences in overall size and ellipticity. With increasing chain length, the distribution of ρ for pairs of random structures is skewed to higher values, but the value for the best 1% of the comparisons rises only slowly with the number of residues. This level is close to an intrinsic cutoff between similar and dissimilar comparisons, namely the maximal scaled ρ possible for the two structures to be more similar to each other than one is to the other's mirror image. The intrinsic cutoff is independent of the number of residues or points being compared. For proteins having fewer than 100 residues, the 1% ρ falls below the intrinsic cutoff, so that for very small proteins, geometrically significant similarity can often occur by chance. We believe these ideas will be helpful in judging success in NMR structure determination and protein folding modeling. © 1995 Wiley‐Liss, Inc.
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