Monte Carlo-extended linear response (MC/ELR) calculations are used to examine the binding of efavirenz analogues with the K103N mutant of HIV-1 reverse transcriptase (HIVRT). A regression equation previously reported for the wild type (WT) enzyme is shown to predict 47 experimental activities for the K103N mutant with a q
2=0.55 and avg error of only 0.46 kcal/mol. Further analysis identifies the key features for binding to the K103N mutant: ligand flexibility, burial of hydrophobic surface area, and protein–ligand van der Waals interactions.
Robert C. Rizzo, Marina Udier–Blagović, Deping Wang, Edward K. Watkins, Marilyn B. Kroeger Smith, Richard H. Smith, Julian Tirado‐Rives, William L. Jorgensen
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