The coordinates of the X-ray crysta

The coordinates of the X-ray crystal structure of the aromatase/ androstenedione complex (PDB code 3EQM) were downloaded from the Protein Databank (http://www.rcsb.org) and imported into the modeling program SYBYL (version 8.0; Tripos, St. Louis, MO). All non-protein components were deleted and hydrogen atoms were added to the protein structure. Partial charges were assigned according to the Amber library and the positions of the added hydrogen atoms were optimized by molecular mechanics minimization that kept the positions of the heavy atoms static.42 Energy minimization was performed with the Powell method in combination with the Amber7 FF99 force field, a distance-dependent dielectric constant of 4, and a convergence criterion of 0.05 kcal/(mol Å). The molecular structures of inhibitors were also prepared in SYBYL and the conformational energy of each structure was minimized by molecular mechanics (MMFF94s force field, MMFF94 charges, and distance-dependent dielectric constant of 4) using the conjugate gradient method and a termination criterion of 0.01 kcal/(mol Å).
Inhibitor structures were computationally docked into the enzyme’s binding site using the program GOLD (version 5.0.1.; CCDC, Cambridge, UK). GOLD operates with a genetic search algorithm and allows for complete ligand and partial binding site flexibility.43 All four scoring functions (GoldScore, ChemScore, ASP, and ChemPLP) were tested and various sizes and centers of the docking sphere were evaluated. The settings for the genetic algorithm runs were kept at their default values (population size: 100, selection pressure: 1.1; number of operations: 100,000, the number of is- lands: 5, niche size: 2, probability for migration, mutation, and crossover: 10%, 95%, and 95%, respectively). For each ligand, 30 runs were performed under identical conditions.