Roles of Conformational and Positional Adaptability in Structure-based Design of TMC125-R165335 (etravirine) and Related Non-nucleoside Reverse Transcriptase Inhibitors That Are Highly Potent and Effective Against Wild-type and Drug-resistant HIV-1...

Overview

Journal J Med Chem

Publisher American Chemical Society

Specialty Chemistry

Date 2004 Apr 30

PMID 15115397

Citations 157

Authors

Kalyan Das

Arthur D Clark Jr

Paul J Lewi

Jan Heeres

Marc R de Jonge

Lucien M H Koymans

H Maarten Vinkers

Frederik Daeyaert

Donald W Ludovici

Michael J Kukla

Bart De Corte

Robert W Kavash

Chih Y Ho

Hong Ye

Mark A Lichtenstein

Koen Andries

Rudi Pauwels

Marie-Pierre de Bethune

Paul L Boyer

Patrick Clark

Stephen H Hughes

Paul A J Janssen

Eddy Arnold

Affiliations

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Abstract

Anti-AIDS drug candidate and non-nucleoside reverse transcriptase inhibitor (NNRTI) TMC125-R165335 (etravirine) caused an initial drop in viral load similar to that observed with a five-drug combination in naïve patients and retains potency in patients infected with NNRTI-resistant HIV-1 variants. TMC125-R165335 and related anti-AIDS drug candidates can bind the enzyme RT in multiple conformations and thereby escape the effects of drug-resistance mutations. Structural studies showed that this inhibitor and other diarylpyrimidine (DAPY) analogues can adapt to changes in the NNRTI-binding pocket in several ways: (1). DAPY analogues can bind in at least two conformationally distinct modes; (2). within a given binding mode, torsional flexibility ("wiggling") of DAPY analogues permits access to numerous conformational variants; and (3). the compact design of the DAPY analogues permits significant repositioning and reorientation (translation and rotation) within the pocket ("jiggling"). Such adaptations appear to be critical for potency against wild-type and a wide range of drug-resistant mutant HIV-1 RTs. Exploitation of favorable components of inhibitor conformational flexibility (such as torsional flexibility about strategically located chemical bonds) can be a powerful drug design concept, especially for designing drugs that will be effective against rapidly mutating targets.

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