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Protein structure comparison by alignment of distance matrices.通过距离矩阵比对进行蛋白质结构比较。
J Mol Biol. 1993 Sep 5;233(1):123-38. doi: 10.1006/jmbi.1993.1489.
2
Many of the immunoglobulin superfamily domains in cell adhesion molecules and surface receptors belong to a new structural set which is close to that containing variable domains.细胞黏附分子和表面受体中的许多免疫球蛋白超家族结构域属于一个新的结构组,该结构组与包含可变结构域的结构组相近。
J Mol Biol. 1994 May 13;238(4):528-39. doi: 10.1006/jmbi.1994.1312.
3
Average core structures and variability measures for protein families: application to the immunoglobulins.蛋白质家族的平均核心结构和变异性度量:在免疫球蛋白中的应用。
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Comparison of protein structures.蛋白质结构的比较
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Protein structure alignment.蛋白质结构比对
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6
Efficient detection of three-dimensional structural motifs in biological macromolecules by computer vision techniques.利用计算机视觉技术高效检测生物大分子中的三维结构基序。
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A method for multiple superposition of structures.一种结构多重叠加的方法。
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On the multiple simultaneous superposition of molecular structures by rigid body transformations.关于通过刚体变换对分子结构进行多重同时叠加
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抗体分子的不变坐标系统:VL和VH结构域“标准”Cα框架的预测。

The invariant system of coordinates of antibody molecules: prediction of the "standard" C alpha framework of VL and VH domains.

作者信息

Gelfand I M, Kister A E, Leshchiner D

机构信息

Department of Mathematics, Rutgers University, New Brunswick, NJ 08903, USA.

出版信息

Proc Natl Acad Sci U S A. 1996 Apr 16;93(8):3675-8. doi: 10.1073/pnas.93.8.3675.

DOI:10.1073/pnas.93.8.3675
PMID:8622995
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC39670/
Abstract

A new approach of comparing protein structures that does not involve the procedure of superposition is suggested. An invariant system of coordinates for immunoglobulin molecules that is based on the geometrical symmetry inherent to the variable domain light-chain (VL)-heavy-chain (VH) complex is described. The coordinates of the Calpha atoms in 22 immunoglobulin structures are calculated in the invariant system of coordinates. We found that 76 identical positions in this Calpha framework are symmetrical about the twofold axis. Comparison of the identical positions in these molecules allows us to select 96 positions in the light chains and 87 positions in the heavy chains whose Calpha atom coordinates are approximately the same. To check whether the average coordinates of Calpha atoms in these positions complies with the stereochemical requirements, we calculated Calpha-Calpha distances. Seventy-three positions of the light chains and 72 positions of the heavy chains satisfy the Calpha-Calpha distance criterion. The Calpha atoms in these positions are used for constructing the "standard" Calpha framework of VL and VH complexes. The average coordinates of Calpha atoms are presented.

摘要

提出了一种不涉及叠加过程的比较蛋白质结构的新方法。描述了一种基于可变域轻链(VL)-重链(VH)复合物固有几何对称性的免疫球蛋白分子坐标不变系统。在该坐标不变系统中计算了22种免疫球蛋白结构中Cα原子的坐标。我们发现,在这个Cα框架中有76个相同位置关于二重轴对称。比较这些分子中的相同位置,使我们能够在轻链中选择96个位置,在重链中选择87个位置,其Cα原子坐标大致相同。为了检查这些位置上Cα原子的平均坐标是否符合立体化学要求,我们计算了Cα-Cα距离。轻链的73个位置和重链的72个位置满足Cα-Cα距离标准。这些位置上的Cα原子用于构建VL和VH复合物的“标准”Cα框架。给出了Cα原子的平均坐标。