| Literature DB >> 9197981 |
M Font1, A Monge, E Alvarez, A Cuartero, M J Losa, M J Fidalgo, C SanMartín, E Nadal, I Ruiz, I Merino, J J Martínez-Irujo, E Alberdi, E Santiago, I Prieto, J J Lasarte, P Sarobe, F Borrás.
Abstract
The synthesis and preliminary evaluation of new quinoline and quinoxaline derivatives (obtained by applying the original Reissert method, conveniently modified) as HIV-1 Reverse Transcriptase (RT) inhibitors are presented in this paper; likewise, the first structure-activity relationships are also proposed. Propyl 2-cyano-1(2H)-quinolin-carboxylate 2e, isopropyl 2-cyano-1 (2H)-quinolincarboxylate 2f, butyl 2-cyano-1 (2H)-quinolincarboxylate 2g and isobutyl 2-cyano-1 (2H)-quinolincarboxylate 2h have been selected as lead compounds. These compounds are active against the HIV-1 RT mutant type P236L (2f, IC50 = 1.2 microM) and present activity as anti-infective agents in HLT41acZ-1IIIB cells, showing no cytotoxicity at the active concentrations.Entities:
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Year: 1997 PMID: 9197981
Source DB: PubMed Journal: Drug Des Discov ISSN: 1026-7921