A multilayer dynamic perturbation analysis method for predicting ligand-protein interactions

Lin Gu; Bin Li; Dengming Ming

doi:10.1186/s12859-022-04995-2

A multilayer dynamic perturbation analysis method for predicting ligand-protein interactions

BMC Bioinformatics. 2022 Nov 2;23(1):456. doi: 10.1186/s12859-022-04995-2.

Authors

Lin Gu¹, Bin Li¹, Dengming Ming²

Affiliations

¹ College of Biotechnology and Pharmaceutical Engineering, Nanjing Tech University, Biotech Building Room B1-404, 30 South Puzhu Road, Jiangbei New District, Nanjing City, 211816, Jiangsu, People's Republic of China.
² College of Biotechnology and Pharmaceutical Engineering, Nanjing Tech University, Biotech Building Room B1-404, 30 South Puzhu Road, Jiangbei New District, Nanjing City, 211816, Jiangsu, People's Republic of China. dming@njtech.edu.cn.

Abstract

Background: Ligand-protein interactions play a key role in defining protein function, and detecting natural ligands for a given protein is thus a very important bioengineering task. In particular, with the rapid development of AI-based structure prediction algorithms, batch structural models with high reliability and accuracy can be obtained at low cost, giving rise to the urgent requirement for the prediction of natural ligands based on protein structures. In recent years, although several structure-based methods have been developed to predict ligand-binding pockets and ligand-binding sites, accurate and rapid methods are still lacking, especially for the prediction of ligand-binding regions and the spatial extension of ligands in the pockets.

Results: In this paper, we proposed a multilayer dynamics perturbation analysis (MDPA) method for predicting ligand-binding regions based solely on protein structure, which is an extended version of our previously developed fast dynamic perturbation analysis (FDPA) method. In MDPA/FDPA, ligand binding tends to occur in regions that cause large changes in protein conformational dynamics. MDPA, examined using a standard validation dataset of ligand-protein complexes, yielded an averaged ligand-binding site prediction Matthews coefficient of 0.40, with a prediction precision of at least 50% for 71% of the cases. In particular, for 80% of the cases, the predicted ligand-binding region overlaps the natural ligand by at least 50%. The method was also compared with other state-of-the-art structure-based methods.

Conclusions: MDPA is a structure-based method to detect ligand-binding regions on protein surface. Our calculations suggested that a range of spaces inside the protein pockets has subtle interactions with the protein, which can significantly impact on the overall dynamics of the protein. This work provides a valuable tool as a starting point upon which further docking and analysis methods can be used for natural ligand detection in protein functional annotation. The source code of MDPA method is freely available at: https://github.com/mingdengming/mdpa .

Keywords: DPA; Dynamics perturbation analysis; Ligand spatial extension; Ligand–protein interaction; Multilayer.

MeSH terms

Algorithms*
Binding Sites
Ligands
Protein Binding
Protein Conformation
Proteins* / chemistry
Reproducibility of Results

Substances

Ligands
Proteins

Grants and funding

2019YFA0905700, 2021YFC2102700/National Key Research and Development Program of China