Abstract

Computational methodology promises to revolutionize the process of designing drugs and antiviral agents. It has the potential to significantly reduce the time and costs associated with 1) the identification and ranking of potential lead compounds; and 2) the enhancement of their specificity and potency. the retroviral proteases present an important and suitable challenge to develop and improve our ability to use computer based techniques in designing appropriate inhibitors. The objectives of this research are to advance our procedures for the automated docking of substrates to proteins into a mature tool with which to aid in the drug design cycle of anti-retroviral agents. Initially we will extend the capabilities and efficiency of our docking algorithm. We will explore methods of incorporating limited protein mobility in the flaps of the aspartic proteases in order to better model the interaction of these target proteins with candidate inhibitors. We will also optimize the force field used in the docking so that the computed energetics of the simulation will accurately represent experimentally observed inhibitor interactions. Our goal in this phase is to allow the ranking of the inhibitory efficacy of trial drugs based on calculated energies of binding. In close collaboration with the other members of this program project, we will test and rank trial drugs using our docking protocol. Our initial targets will be the HIV protease and models for the FIV protease. Candidate drugs will be tested against both of these protease models in order to identify leads which may have more viability against mutational drift. Differential binding of drugs to retroviral proteases and to host aspartic proteases will be compared to enhance drug specificity. We will develop and test novel rational drug design strategies that will use recent computational algorithms to suggest novel drug candidates. Two different applications incorporating the Metropolis and the genetic algorithms will yield entirely new avenues of drug morphology. In our first approach we will use these algorithms to mutate drugs during the docking simulation. In the second approach we will grow and recombine fragments to yield new combinations. The tools that will be developed, tested and applied in this project should serve as a critical component in a state-of-the-art drug design cycle and will be made available to the scientific community.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Program Projects (P01)
Project #
5P01GM048870-09
Application #
6340972
Study Section
Project Start
2000-09-01
Project End
2001-08-31
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
9
Fiscal Year
2000
Total Cost
$113,837
Indirect Cost

  Institution

Name
Scripps Research Institute
Department
Type
DUNS #
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Morris, Garrett M; Green, Luke G; Radi?, Zoran et al. (2013) Automated docking with protein flexibility in the design of femtomolar ""click chemistry"" inhibitors of acetylcholinesterase. J Chem Inf Model 53:898-906
Breuer, Sebastian; Sepulveda, Homero; Chen, Yu et al. (2011) A cleavage enzyme-cytometric bead array provides biochemical profiling of resistance mutations in HIV-1 Gag and protease. Biochemistry 50:4371-81
Chang, Max W; Torbett, Bruce E (2011) Accessory mutations maintain stability in drug-resistant HIV-1 protease. J Mol Biol 410:756-60
Chang, Max W; Giffin, Michael J; Muller, Rolf et al. (2010) Identification of broad-based HIV-1 protease inhibitors from combinatorial libraries. Biochem J 429:527-32
Chang, Max W; Ayeni, Christian; Breuer, Sebastian et al. (2010) Virtual screening for HIV protease inhibitors: a comparison of AutoDock 4 and Vina. PLoS One 5:e11955
Sundstrom, Magnus; Chatterji, Udayan; Schaffer, Lana et al. (2008) Feline immunodeficiency virus OrfA alters gene expression of splicing factors and proteasome-ubiquitination proteins. Virology 371:394-404
Nelson, Josh D; Kinkead, Heather; Brunel, Florence M et al. (2008) Antibody elicited against the gp41 N-heptad repeat (NHR) coiled-coil can neutralize HIV-1 with modest potency but non-neutralizing antibodies also bind to NHR mimetics. Virology 377:170-83
Giffin, Michael J; Heaslet, Holly; Brik, Ashraf et al. (2008) A copper(I)-catalyzed 1,2,3-triazole azide-alkyne click compound is a potent inhibitor of a multidrug-resistant HIV-1 protease variant. J Med Chem 51:6263-70
Huey, Ruth; Morris, Garrett M; Olson, Arthur J et al. (2007) A semiempirical free energy force field with charge-based desolvation. J Comput Chem 28:1145-52
Heaslet, Holly; Rosenfeld, Robin; Giffin, Mike et al. (2007) Conformational flexibility in the flap domains of ligand-free HIV protease. Acta Crystallogr D Biol Crystallogr 63:866-75

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