Structural and Energetic Analyses of the Effects of the K103N Mutation of HIV-1 Reverse Transcriptase on Efavirenz Analogues

Marina Udier–Blagović; Julian Tirado‐Rives; William L. Jorgensen

doi:10.1021/jm0303507

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Structural and Energetic Analyses of the Effects of the K103N Mutation of HIV-1 Reverse Transcriptase on Efavirenz Analogues

Journal of Medicinal Chemistry 47(9): 2389-2392

Article 2004 English

Authors

MU
Marina Udier–Blagović
JT
Julian Tirado‐Rives
William L. Jorgensen
Yale University

Abstract

1 min read

The effect of the K103N mutation of HIV-1 reverse transcriptase (RT) on the activity of efavirenz analogues was studied via Monte Carlo/free energy perturbation calculations. The relative fold resistance energies indicate that efavirenz binds to K103N RT in a manner similar to the wild-type enzyme. The improved performance of the quinazolinones against the mutant enzyme is attributed to formation of a more optimal hydrogen-bonding network with bridging water molecules between the ligands and Glu138.

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