35.1 INTRODUCTION

Docking is an attempt to determine whether two molecules interact with each other, and to find the best match between these two molecules. Biocomputational “docking”, thus, predicts the preferred orientation of one molecule (e.g., protein) bound to another molecule (a ligand) in a lock‐and‐key manner. The particular orientation necessitates overall minimum free energy (ΔG). Docking is necessary because it is a key to rational and sensible drug design. In the process of docking, all intermolecular forces (i.e., H‐bonding, hydrophobicity, dipole–dipole interaction, Van der Waals forces, electrostatic interactions and intra‐molecular forces) and the bond features (i.e., bond length, bond angle, dihedral angle) are taken into account. Docking can be rigid, or there are flexible types. The docking studies are categorized broadly into protein–ligand docking; protein–protein docking; and protein–nucleic acid docking.

35.2 OBJECTIVE

To find the best binding poses of the receptor–ligand complex, based on energy minima of the system.

35.3 PROCEDURE