Abstract

Our program proposes to design and synthesize compounds that inhibit the action of HIV Integrase. At present, integrase is the only HIV enzyme for which clinically useful inhibitors are not available. Given the recent success of combined therapy targeting reverse transcriptase and protease simultaneously, it is highly desirable to include the third target HIV integrase. We propose to carry out a coordinated series of experiment to develop such inhibitors. Our group brings unique expertise and background data to this effort. We have improved the resolution of the structure of the integrase catalytic domain substantially, providing a point of departure for structure-guided design of inhibitors. Using assays based on preintegration complexes isolated from HIV infected cells, we have identified particularly potent integrase inhibitors. We are presently attempting to form various co- crystal complexes of these inhibitors bound to the integrase catalytic domain. We plan to use integrase-inhibitor structures to design improved inhibitors, which will then be tested . Effective new inhibitors will then be analyzed as co-crystals with the integrase catalytic domain. We hope that several cycles of synthesis testing, co-crystallization and new inhibitor design will yield clinically useful drugs. While this structure-guided design strategy forms the center of our effort, we have also prepared other routes to the achievement of the goal of creating useful inhibitors. We use the unliganded integrase structure to """"""""discover and grow"""""""" compounds that bind the active site. Such molecules will be synthesized and tested. The structures of lead drugs will identify related compounds to synthesize and test. Natural products with structures related to known inhibitors will be tested for inhibition of integrase. Finally, integrase variants insensitive to drugs will be isolated by genetic means. The locations of such changes in the integrase structure will provide information on likely locations of drug binding sites. This information will be incorporated into the design of improved small molecule inhibitors.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Program Projects (P01)
Project #
5P01GM056553-05
Application #
6386770
Study Section
Special Emphasis Panel (ZGM1-AIDS-2 (01))
Program Officer
Cassatt, James
Project Start
1997-08-01
Project End
2003-07-31
Budget Start
2001-08-01
Budget End
2003-07-31
Support Year
5
Fiscal Year
2001
Total Cost
$928,835
Indirect Cost

  Institution

Name
Salk Institute for Biological Studies
Department
Type
DUNS #
005436803
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Deng, Jinxia; Sanchez, Tino; Neamati, Nouri et al. (2006) Dynamic pharmacophore model optimization: identification of novel HIV-1 integrase inhibitors. J Med Chem 49:1684-92
Brigo, A; Mustata, G Iurcu; Briggs, J M et al. (2005) Discovery of HIV-1 integrase inhibitors through a novel combination of ligand and structure-based drug design. Med Chem 1:263-75
Lee, Matthew C; Deng, Jinxia; Briggs, James M et al. (2005) Large-scale conformational dynamics of the HIV-1 integrase core domain and its catalytic loop mutants. Biophys J 88:3133-46
Brigo, Alessandro; Lee, Keun Woo; Fogolari, Federico et al. (2005) Comparative molecular dynamics simulations of HIV-1 integrase and the T66I/M154I mutant: binding modes and drug resistance to a diketo acid inhibitor. Proteins 59:723-41
Brigo, Alessandro; Lee, Keun Woo; Iurcu Mustata, Gabriela et al. (2005) Comparison of multiple molecular dynamics trajectories calculated for the drug-resistant HIV-1 integrase T66I/M154I catalytic domain. Biophys J 88:3072-82
Mustata, Gabriela Iurcu; Brigo, Alessandro; Briggs, James M (2004) HIV-1 integrase pharmacophore model derived from diverse classes of inhibitors. Bioorg Med Chem Lett 14:1447-54
Adesokan, Adeyemi A; Roberts, Victoria A; Lee, Keun Woo et al. (2004) Prediction of HIV-1 integrase/viral DNA interactions in the catalytic domain by fast molecular docking. J Med Chem 47:821-8
Lerch, Melissa L; Harper, Mary Kay; Faulkner, D John (2003) Brominated polyacetylenes from the Philippines sponge Diplastrella sp. J Nat Prod 66:667-70
Gao, Kui; Gorelick, Robert J; Johnson, Donald G et al. (2003) Cofactors for human immunodeficiency virus type 1 cDNA integration in vitro. J Virol 77:1598-603
Hu, Wen-Yuan; Myers, Christopher P; Kilzer, Jennifer M et al. (2002) Inhibition of retroviral pathogenesis by RNA interference. Curr Biol 12:1301-11

Showing the most recent 10 out of 42 publications