Developing a methodology to simulate flexible complete docking and specific mutation in the primary structure and its applications to study interaction protein-protein, protein-ligand and resistance of pathogenesis and drugs

Abstract

There are several methods/software to simulate molecular docking; those that have been implemented use different force fields and algorithms. Different approximations exist depending which type of degrees of freedom are to be considered, and this includes rigid docking where protein and ligand are rigid, semi-flexible where only a selected set of side-chains of the protein are allowed to move, or fully flexible where all the protein (including the backbone) and the ligand are allowed to change their conformation The mains objectives of this research project are: extend and improve the methodology GANM developed by a regular research project (Proc. 2007/05696-2). The new version (extended) will be able to simulate docking of protein-protein and it will be able study the effect of specific mutations in the context of docking. (AU)