Rackovsky S
Department of Biophysics, School of Medicine and Dentistry, University of Rochester, New York 14642.
Proteins. 1990;7(4):378-402. doi: 10.1002/prot.340070409.
We address herein the problem of delineating the relationships between the known protein structures. In order to study this problem, methods have been developed to represent arbitrarily sized fragments of biopolymer backbone, and to compare distributions of such fragments. These methods are applied to a classification of 123 structures representing the entire set of known x-ray structures. The resulting data are analyzed (on the four-C alpha length scale) to determine both the large-scale organization of the set of known structures (i.e., the relationships between large groups of structures, each comprised of proteins that are structurally related) and its local structure (i.e., the quantitative degree of similarity between any two specific structures). It is shown that the set of structures forms a continuum of structural types, ranging from all-helical to all-sheet/barrel proteins. It is further demonstrated that the density of protein structures is not uniform across this continuum, but rather that structures cluster in certain regions, separated by regions of lower population. The properties of the various regions of the structural space are determined. The existence is demonstrated of strong quantitative correlations between the contents of different types of four-C alpha fragments within protein structures, which imply significant constraints on the types of architecture that can occur in proteins. Analysis of the distribution of structures demonstrates some hitherto unsuspected similarities and suggests that, in some circumstances, neither structural similarity nor sequence homology may be necessary conditions for evolutionary relationship between proteins. It is also suggested that these unsuspected similarities may imply similar folding mechanisms for structures of apparently different global architecture. Cases are also noted in which apparently similar structures may fold by different mechanisms. The connection between structure and dynamic properties is discussed, and a possible role of dynamics in the evolution of protein structures is suggested. The sensitivity of the methods presented herein to anomalies of structure refinement is demonstrated. It is suggested that the present results provide a framework for analyzing experimental results on structural similarity obtained using vibrational circular dichroism spectra, which are sensitive to local backbone structure.
我们在此探讨描绘已知蛋白质结构之间关系的问题。为了研究这个问题,已开发出一些方法来表示生物聚合物主链的任意大小片段,并比较这些片段的分布。这些方法被应用于对代表已知X射线结构全集的123个结构进行分类。对所得数据(在四个Cα长度尺度上)进行分析,以确定已知结构集的大规模组织(即大的结构组之间的关系,每个结构组由结构相关的蛋白质组成)及其局部结构(即任意两个特定结构之间的定量相似程度)。结果表明,结构集形成了一个结构类型的连续体,范围从全螺旋蛋白到全β折叠/桶状蛋白。进一步证明,蛋白质结构的密度在这个连续体上并不均匀,而是在某些区域聚集,被低丰度区域隔开。确定了结构空间各个区域的特性。证明了蛋白质结构中不同类型的四个Cα片段含量之间存在强定量相关性,这意味着对蛋白质中可能出现的结构类型有显著限制。对结构分布的分析揭示了一些迄今未被怀疑的相似性,并表明在某些情况下,结构相似性和序列同源性都可能不是蛋白质之间进化关系的必要条件。还表明,这些未被怀疑的相似性可能意味着表面上不同整体结构的结构具有相似的折叠机制。也注意到了一些情况,即表面上相似的结构可能通过不同的机制折叠。讨论了结构与动态特性之间的联系,并提出了动力学在蛋白质结构进化中的可能作用。证明了本文提出的方法对结构精修异常的敏感性。建议目前的结果为分析使用振动圆二色光谱获得的关于结构相似性的实验结果提供一个框架,振动圆二色光谱对局部主链结构敏感。
