Abstract

HIV-1 protease is a promising therapeutic target for antiviral therapy in AIDS patients since it plays a criticalrole in the virus life cycle by processing the viral Gag and Gag-Pol polyproteins into structural and functionalproteins essential for viral maturation. Chemotherapy based on the combination of protease and reversetranscriptase inhibitors has been remarkably successful in reducing the mortality rates in AIDS patients.However, under the selective pressure of drug therapy, the emergence of many viable multidrug-resistant(MDR) protease variants is posing a great challenge to the efficacy of currently available protease inhibitors.The PPG team has been pursuing a structure- and informatics-based strategy to design and evaluate newprotease inhibitor libraries targeting ensembles of HIV-1 proteases. The computational groups at MIT (Tidorlab) and CARB (Gilson lab) have designed inhibitor libraries using databases of commercially availablecompounds; these libraries are referred to as the MIT and CARB libraries, respectively. The core group atUMASS (Rana lab) has carried out the chemical synthesis of designed inhibitor libraries and tested theiractivities against wild-type and three MDR protease variants. In addition, the Rana lab has designed,synthesized and evaluated 2 novel series of protease inhibitors with highly potent activities against wild-typeand MDR variants. As a core component of the PPG, the Rana lab has synthesized hundreds of newinhibitors and evaluated their activities against wild-type and three MDR protease variants. The current PPGteam, comprising a HIV drug-resistance analysis and database group (Shafer lab), a molecular virologygroup (Swanstrom lab), a structural biology group (Schiffer lab), a computational group (Tidor lab), and achemical synthesis and screening group (Core A, Rana lab), is continuing to pursue the overall goals ofdesigning, synthesizing and evaluating new protease inhibitor libraries targeting ensembles of MDRproteases. These designed inhibitors will likely be less susceptible to drug resistance, thus improving thelong-term efficacy of HIV-1 protease inhibitors in preventing the progression of HIV-1 infections. The majorgoal of the core facility is to synthesize and screen computationally designed inhibitor libraries against wildtypeand selected MDR variants of protease. The core facility consists of three scientists who areresponsible for synthesizing, screening and maintaining instruments.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Program Projects (P01)
Project #
2P01GM066524-06
Application #
7356923
Study Section
Special Emphasis Panel (ZRG1-AARR-A (40))
Project Start
2007-08-01
Project End
2012-07-31
Budget Start
2007-08-01
Budget End
2008-08-31
Support Year
6
Fiscal Year
2007
Total Cost
$430,118
Indirect Cost

  Institution

Name
University of Massachusetts Medical School Worcester
Department
Type
DUNS #
603847393
City
Worcester
State
MA
Country
United States
Zip Code
01655

  Publications

Zhou, Hao; Li, Shangyang; Badger, John et al. (2015) Modulation of HIV protease flexibility by the T80N mutation. Proteins 83:1929-39
Lee, Sook-Kyung; Cheng, Nancy; Hull-Ryde, Emily et al. (2013) A sensitive assay using a native protein substrate for screening HIV-1 maturation inhibitors targeting the protease cleavage site between the matrix and capsid. Biochemistry 52:4929-40
Shen, Yang; Altman, Michael D; Ali, Akbar et al. (2013) Testing the substrate-envelope hypothesis with designed pairs of compounds. ACS Chem Biol 8:2433-41
Silver, Nathaniel W; King, Bracken M; Nalam, Madhavi N L et al. (2013) Efficient Computation of Small-Molecule Configurational Binding Entropy and Free Energy Changes by Ensemble Enumeration. J Chem Theory Comput 9:5098-5115
Foulkes-Murzycki, Jennifer E; Rosi, Christina; Kurt Yilmaz, Nese et al. (2013) Cooperative effects of drug-resistance mutations in the flap region of HIV-1 protease. ACS Chem Biol 8:513-8
Schiffer, Celia (2013) Interview with Celia Schiffer. Future Med Chem 5:1193-7
Nalam, Madhavi N L; Ali, Akbar; Reddy, G S Kiran Kumar et al. (2013) Substrate envelope-designed potent HIV-1 protease inhibitors to avoid drug resistance. Chem Biol 20:1116-24
Mittal, Seema; Bandaranayake, Rajinthna M; King, Nancy M et al. (2013) Structural and thermodynamic basis of amprenavir/darunavir and atazanavir resistance in HIV-1 protease with mutations at residue 50. J Virol 87:4176-84
King, Nancy M; Prabu-Jeyabalan, Moses; Bandaranayake, Rajintha M et al. (2012) Extreme entropy-enthalpy compensation in a drug-resistant variant of HIV-1 protease. ACS Chem Biol 7:1536-46
Alvizo, Oscar; Mittal, Seema; Mayo, Stephen L et al. (2012) Structural, kinetic, and thermodynamic studies of specificity designed HIV-1 protease. Protein Sci 21:1029-41

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