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Acyclic nucleoside thiophosphonates as potent inhibitors of HIV and HBV replication.


ABSTRACT: 9-[2-(Thiophosphonomethoxy)ethyl]adenine 3 and (R)-9-[2-(Thiophosphonomethoxy)propyl]adenine 4 were synthesized as the first thiophosphonate nucleosides bearing a sulfur atom at the ?-position of the acyclic nucleoside phosphonates PMEA and PMPA. Thiophosphonates S-PMEA 3 and S-PMPA 4 were evaluated for in vitro activity against HIV-1 (subtypes A to G), HIV-2 and HBV-infected cells, and found to exhibit potent antiretroviral activity. We showed that their diphosphate forms S-PMEApp 5 and S-PMPApp 6 are readily incorporated by wild-type (WT) HIV-1 RT into DNA and act as DNA chain terminators. Compounds 3 and 4 were evaluated for in vitro activity against a broad panel of DNA and RNA viruses and displayed beside HIV a moderate activity against herpes simplex virus and vaccinia viruses. In order to measure enzymatic stabilities of the target derivatives 3 and 4, kinetic data and decomposition pathways were studied at 37 °C in several media.

SUBMITTER: Barral K 

PROVIDER: S-EPMC7115536 | biostudies-literature | 2011 Sep

REPOSITORIES: biostudies-literature

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Acyclic nucleoside thiophosphonates as potent inhibitors of HIV and HBV replication.

Barral Karine K   Weck Clément C   Payrot Nadine N   Roux Loic L   Durafour Céline C   Zoulim Fabien F   Neyts Johan J   Balzarini Jan J   Canard Bruno B   Priet Stéphane S   Alvarez Karine K  

European journal of medicinal chemistry 20110701 9


9-[2-(Thiophosphonomethoxy)ethyl]adenine 3 and (R)-9-[2-(Thiophosphonomethoxy)propyl]adenine 4 were synthesized as the first thiophosphonate nucleosides bearing a sulfur atom at the α-position of the acyclic nucleoside phosphonates PMEA and PMPA. Thiophosphonates S-PMEA 3 and S-PMPA 4 were evaluated for in vitro activity against HIV-1 (subtypes A to G), HIV-2 and HBV-infected cells, and found to exhibit potent antiretroviral activity. We showed that their diphosphate forms S-PMEApp 5 and S-PMPAp  ...[more]

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