Design, synthesis, and biological and structural evaluations of novel HIV-1 protease inhibitors to combat drug resistance
Authors
Parai, Maloy KumarHuggins, David J.
Cao, Hong
Nalam, Madhavi N. L.
Ali, Akbar
Schiffer, Celia A.
Tidor, Bruce
Rana, Tariq M.
UMass Chan Affiliations
Department of Biochemistry and Molecular PharmacologyDocument Type
Journal ArticlePublication Date
2012-07-26Keywords
Drug DesignDrug Resistance, Viral
HIV Protease
HIV Protease Inhibitors
HIV-1
Biochemistry, Biophysics, and Structural Biology
Pharmacology, Toxicology and Environmental Health
Metadata
Show full item recordAbstract
A series of new HIV-1 protease inhibitors (PIs) were designed using a general strategy that combines computational structure-based design with substrate-envelope constraints. The PIs incorporate various alcohol-derived P2 carbamates with acyclic and cyclic heteroatomic functionalities into the (R)-hydroxyethylamine isostere. Most of the new PIs show potent binding affinities against wild-type HIV-1 protease and three multidrug resistant (MDR) variants. In particular, inhibitors containing the 2,2-dichloroacetamide, pyrrolidinone, imidazolidinone, and oxazolidinone moieties at P2 are the most potent with K(i) values in the picomolar range. Several new PIs exhibit nanomolar antiviral potencies against patient-derived wild-type viruses from HIV-1 clades A, B, and C and two MDR variants. Crystal structure analyses of four potent inhibitors revealed that carbonyl groups of the new P2 moieties promote extensive hydrogen bond interactions with the invariant Asp29 residue of the protease. These structure-activity relationship findings can be utilized to design new PIs with enhanced enzyme inhibitory and antiviral potencies.Source
J Med Chem. 2012 Jul 26;55(14):6328-41. Epub 2012 Jul 13. Link to article on publisher's site
DOI
10.1021/jm300238hPermanent Link to this Item
http://hdl.handle.net/20.500.14038/26018PubMed ID
22708897Related Resources
Link to Article in PubMedae974a485f413a2113503eed53cd6c53
10.1021/jm300238h