Basic quinolinonyl diketo acid derivatives as inhibitors of HIV integrase and their activity against RNase H function of reverse transcriptase
- COSTI R
- MÉTIFIOT M
- CHUNG S
- CUZZUCOLI CRUCITTI G
- MADDALI K
- PESCATORI L
- MESSORE A
- MADIA VN
- PUPO G
- SCIPIONE L
- TORTORELLA S
- DI LEVA FS
- COSCONATI S
- MARINELLI L
- NOVELLINO E
- LE GRICE SF
- CORONA A
- POMMIER Y
- MARCHAND C
- DI SANTO R.
Publication date
January 2014
DOI Publisher
American Chemical Society (ACS) ISSN
0022-2623 Citation count (estimate)
19Abstract
A series of antiviral basic quinolinonyl diketo acid derivatives were developed as inhibitors of HIV-1 IN. Compounds 12d,f,i inhibited HIV-1 IN with IC50 values below 100 nM for strand transfer and showed a 2 order of magnitude selectivity over 3'-processing. These strand transfer selective inhibitors also inhibited HIV-1 RNase H with low micromolar potencies. Molecular modeling studies based on both the HIV-1 IN and RNase H catalytic core domains provided new structural insights for the future development of these compounds as dual HIV-1 IN and RNase H inhibitors
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