Multi-Body Interactions in Molecular Docking Program Devised with Key Water Molecules in Protein Binding Sites

Wei Xiao; Disha Wang; Zihao Shen; Shiliang Li; Honglin Li

doi:10.3390/molecules23092321

Multi-Body Interactions in Molecular Docking Program Devised with Key Water Molecules in Protein Binding Sites

Molecules. 2018 Sep 11;23(9):2321. doi: 10.3390/molecules23092321.

Authors

Wei Xiao^{1

2}, Disha Wang³, Zihao Shen², Shiliang Li⁴, Honglin Li^{5

6}

Affiliations

¹ School of Information Science and Engineering, East China University of Science and Technology, 130 Meilong Road, Shanghai 200237, China. xiaowei1012163@163.com.
² Shanghai Key Laboratory of New Drug Design, School of Pharmacy, East China University of Science and Technology, 130 Meilong Road, Shanghai 200237, China. xiaowei1012163@163.com.
³ Shanghai Key Laboratory of New Drug Design, School of Pharmacy, East China University of Science and Technology, 130 Meilong Road, Shanghai 200237, China. dishawang@foxmail.com.
⁴ Shanghai Key Laboratory of New Drug Design, School of Pharmacy, East China University of Science and Technology, 130 Meilong Road, Shanghai 200237, China. slli403@163.com.
⁵ School of Information Science and Engineering, East China University of Science and Technology, 130 Meilong Road, Shanghai 200237, China. hlli@ecust.edu.cn.
⁶ Shanghai Key Laboratory of New Drug Design, School of Pharmacy, East China University of Science and Technology, 130 Meilong Road, Shanghai 200237, China. hlli@ecust.edu.cn.

Abstract

Water molecules play an important role in modeling protein-ligand interactions. However, traditional molecular docking methods often ignore the impact of the water molecules by removing them without any analysis or keeping them as a static part of the proteins or the ligands. Hence, the accuracy of the docking simulations will inevitably be damaged. Here, we introduce a multi-body docking program which incorporates the fixed or the variable number of the key water molecules in protein-ligand docking simulations. The program employed NSGA II, a multi-objective optimization algorithm, to identify the binding poses of the ligand and the key water molecules for a protein. To this end, a force-field-based hydration-specific scoring function was designed to favor estimate the binding affinity considering the key water molecules. The program was evaluated in aspects of the docking accuracy, cross-docking accuracy, and screening efficiency. When the numbers of the key water molecules were treated as fixed-length optimization variables, the docking accuracy of the multi-body docking program achieved a success rate of 80.58% for the best RMSD values for the recruit of the ligands smaller than 2.0 Å. The cross-docking accuracy was investigated on the presence and absence of the key water molecules by four protein targets. The screening efficiency was assessed against those protein targets. Results indicated that the proposed multi-body docking program was with good performance compared with the other programs. On the other side, when the numbers of the key water molecules were treated as variable-length optimization variables, the program obtained comparative performance under the same three evaluation criterions. These results indicated that the multi-body docking with the variable numbers of the water molecules was also efficient. Above all, the multi-body docking program developed in this study was capable of dealing with the problem of the water molecules that explicitly participating in protein-ligand binding.

Keywords: multi-body docking; multi-objective optimization; optimization variables; water molecules.

MeSH terms

Algorithms
Binding Sites
Ligands
Models, Molecular
Molecular Docking Simulation
Protein Binding
Proteins / chemistry*
Proteins / metabolism*
Water / chemistry*

Substances

Ligands
Proteins
Water

Grants and funding

2016YFA0502304/National Key Research and Development Program