Ma Bin-Guang, Chen Ling-Ling, Zhang Hong-Yu
Shandong Provincial Research Center for Bioinformatic Engineering and Technique, Center for Advanced Study, Shandong University of Technology, Zibo 255049, PR China.
J Mol Biol. 2007 Jul 13;370(3):439-48. doi: 10.1016/j.jmb.2007.04.051. Epub 2007 May 4.
Protein folding experiments demonstrate that the folding behaviors of many proteins can be roughly classified into two types: two-state kinetics and multi-state kinetics. Although the two types of protein folding kinetics have been observed for a long time, what determines the folding type of a protein is still largely unclear. The present work performed a comparative study based on a dataset of 43 two-state and 42 multi-state folders at different levels of proteins' intrinsic properties from the simplest sequence length to native structure topology. The results show that protein's amino acids composition and the long-range interaction-based topological complexity rather than secondary structure contents are the major determinants of protein folding type. Furthermore, a sequence-based folding type prediction achieved an accuracy of more than 80%. These findings implicate that there is no clear boundary between secondary and tertiary structure formation during the protein folding process and support the existence of a continuum of folding mechanism between the two ends of hierarchic and nucleation folding scenarios.
蛋白质折叠实验表明,许多蛋白质的折叠行为大致可分为两种类型:两态动力学和多态动力学。尽管这两种蛋白质折叠动力学类型已被观察到很长时间,但决定蛋白质折叠类型的因素仍很大程度上不清楚。目前的工作基于一个数据集进行了比较研究,该数据集包含43个两态折叠蛋白和42个多态折叠蛋白,涉及从最简单的序列长度到天然结构拓扑结构等不同层次的蛋白质内在特性。结果表明,蛋白质的氨基酸组成以及基于长程相互作用的拓扑复杂性而非二级结构含量是蛋白质折叠类型的主要决定因素。此外,基于序列的折叠类型预测准确率超过了80%。这些发现表明,在蛋白质折叠过程中,二级结构和三级结构形成之间没有明确的界限,并支持在层次折叠和成核折叠场景两端之间存在连续的折叠机制。