Influenza Virus Neuraminidase Inhibitors: Generation and Comparison of Structure‐Based and Common Feature Pharmacophore Hypotheses and Their Application in Virtual Screening.

Abstract

X-ray crystallographic data of the influenza virus neuraminidase in complex with different inhibitors were used to generate chemical feature-based pharmacophore models of the binding site of this enzyme. The models were built using the software package Catalyst. Pharmacophore hypotheses derived from the 3-D structure of ligands cocrystallized with the enzyme were then compared with automatically generated common feature pharmacophore hypotheses for neuraminidase inhibitors. The latter models were found to contain fewer features and exhibited lower selectivity in virtual screening experiments. Some functions of the inhibitors obviously participate in more than one mode of interaction with the enzyme (charge-charge interaction and hydrogen bond) or form hydrogen bonds to several amino acids. Since such multiple interactions of one chemical function cannot be included into the Catalyst data format, strategies are presented to overcome these limitations. Finally, the results of 3-D database searching experiments using these hypotheses are described.