摘要
提出了一个界面几何约束的多起点蒙特卡罗构象搜索方法,并把这个方法用于三个丝氨酸蛋白酶/短肽抑制剂体系的刚性、部分柔性和全部柔性对接计算中.我们的方法成功地预测出了接近晶体结构的配体构象.与没有几何约束相比。
A multi - start Monte Carlo procedure restrained by surface geometry match is presented and used to dock three serine protease - peptide segment systems. For each of the ligands, one. hundred of initial conformations, which meet given steric and geometric tolerances, are selected randomly. Each of the initial conformations is optimized by a local Monte Carlo procedure which makes a step to a new random step along with the routine of reduction of the radius of gyration R-g of protein - ligand complex according to a given probability. The random step is followed by a local minimization in the total conformational spaces. The radius of gyration R-g of protein - ligand complex characters the quality of geometric fit. Small Rg value corresponds to compact packing and good fit of geometry on the interface. The algorithm successfully predicts the conformations of ligands close to the crystal structures for the three test systems in the docking of rigidity, partial flexibility and total flexibility and the runs display much better convergence properties than the procedure without the guide of geometric fit.
出处
《化学学报》
SCIE
CAS
CSCD
北大核心
2001年第8期1171-1175,共5页
Acta Chimica Sinica
基金
高等院校骨干教师基金,国家重点实验室基金
