Synthesis, biological activity, and crystal structure of potent nonnucleoside inhibitors of HIV-1 reverse transcriptase that retain activity against mutant forms of the enzyme

Author:

Morningstar, M. L.

Roth, T.

Farnsworth, D. W.

Smith, M. K.

Watson, K.

Buckheit, R. W.

Das, K.

Zhang, W. Y.

Arnold, E.

Julias, J. G.

Hughes, S. H.

Michejda, C. J.
Author Address

NCI, Mol Aspects Drug Design Sect, Frederick, MD 21702 USA. NCI, Retroviral Replicat Lab, Frederick, MD 21702 USA. McDaniel Coll, Westminster, MD 21157 USA. So Res Inst, Frederick Res Ctr, Frederick, MD 21701 USA. Rutgers State Univ, Ctr Adv Biotechnol & Med, Piscataway, NJ 08854 USA. Rutgers State Univ, Dept Chem & Chem Biol, Piscataway, NJ 08854 USA.;Farnsworth, DW, NCI, Mol Aspects Drug Design Sect, POB B, Frederick, MD 21702 USA.;farnswor@ncifcrf.gov

Abstract:

In an ongoing effort to develop novel and potent nonnucleoside HIV-1 reverse transcriptase (RT) inhibitors that are effective against the wild type (WT) virus and clinically observed mutants, 1,2-bis-substituted benzimidazoles were synthesized and tested. Optimization of the N1 and C2 positions of benzimidazole led to the development of 1-(2,6-difluorobenzyl)-2-(2,6-difluorophenyl)-4-methylbenzimidazole (1) (IC50 = 0.2 mu M, EC50 = 0.44 mu M, and TC50 >= 100 against WT). This paper describes how substitution on the benzimidazole ring profoundly affects activity. Substituents at the benzimidazole C4 dramatically enhanced potency, while at C5 or C6 substituents were generally detrimental or neutral to activity, respectively. A 7-methyl analogue did not inhibit HIV-1 RT. Determination of the crystal structure of 1 bound to RT provided the basis for accurate modeling of additional analogues, which were synthesized and tested. Several derivatives were nanomolar inhibitors of wild-type virus and were effective against clinically relevant HIV-1 mutants.

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