Sun S
Structural Biochemistry Program, Frederick Biomedical Supercomputing Center, National Cancer Institute, Frederick Cancer Research and Development Center, Maryland 21702, USA.
Biophys J. 1995 Aug;69(2):340-55. doi: 10.1016/S0006-3495(95)79906-4.
We describe a computer algorithm to predict native structures of proteins and peptides from their primary sequences, their known native radii of gyration, and their known disulfide bonding patterns, starting from random conformations. Proteins are represented as simplified real-space main chains with single-bead side chains. Nonlocal interactions are taken from structural database-derived statistical potentials, as in an earlier treatment. Local interactions are taken from simulations of (phi, psi) energy surfaces for each amino acid generated using the Biosym Discover program. Conformational searching is done by a genetic algorithm-based method. Reasonable structures are obtained for melittin (a 26-mer), avian pancreatic polypeptide inhibitor (a 36-mer), crambin (a 46-mer), apamin (an 18-mer), tachyplesin (a 17-mer), C-peptide of ribonuclease A (a 13-mer), and four different designed helical peptides. A hydrogen bond interaction was tested and found to be generally unnecessary for helical peptides, but it helps fold some sheet regions in these structures. For the few longer chains we tested, the method appears not to converge. In those cases, it appears to recover native-like secondary structures, but gets incorrect tertiary folds.
我们描述了一种计算机算法,该算法可从蛋白质和肽的一级序列、已知的天然回转半径以及已知的二硫键连接模式出发,从随机构象开始预测其天然结构。蛋白质被表示为具有单珠侧链的简化实空间主链。非局部相互作用取自结构数据库衍生的统计势,如同早期的处理方法。局部相互作用取自使用Biosym Discover程序生成的每个氨基酸的(φ,ψ)能量表面的模拟。构象搜索通过基于遗传算法的方法进行。对于蜂毒素(一种26肽)、禽胰多肽抑制剂(一种36肽)、胰凝乳蛋白酶原(一种46肽)、蜂毒明肽(一种18肽)、鲎肽(一种17肽)、核糖核酸酶A的C肽(一种13肽)以及四种不同设计的螺旋肽,均获得了合理的结构。对氢键相互作用进行了测试,发现其对于螺旋肽通常并非必需,但有助于这些结构中某些折叠区域的折叠。对于我们测试的少数较长链,该方法似乎未收敛。在这些情况下,它似乎恢复了类似天然的二级结构,但获得了错误的三级折叠。
