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Hybridization of Fluoro-amodiaquine (FAQ) with Pyrimidines: Synthesis and Antimalarial Efficacy of FAQ-Pyrimidines.


ABSTRACT: To evade the possible toxicity associated with the formation of quinone-imine metabolite in amodiaquine (AQ), the para-hydroxyl group was replaced with a -F atom, and the resulting 4'-fluoro-amodiaquine (FAQ) was hybridized with substituted pyrimidines. The synthesized FAQ-pyrimidines displayed better in vitro potency than chloroquine (CQ) against the resistant P. falciparum strain (Dd2), exhibiting up to 47.3-fold better activity (IC50: 4.69 nM) than CQ (IC50: 222 nM) and 2.8-fold better potency than artesunate (IC50: 13.0 nM). Twelve compounds exhibited better antiplasmodial activity than CQ against the CQ-sensitive (NF54) strain. Two compounds were evaluated in vivo against a P. berghei-mouse malaria model. Mechanistic heme-binding studies, computational docking studies against Pf-DHFR and in vitro microsomal stability studies were performed for the representative molecules of the series to assess their antimalarial efficacy.

SUBMITTER: Tripathi M 

PROVIDER: S-EPMC6511959 | biostudies-literature | 2019 May

REPOSITORIES: biostudies-literature

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Hybridization of Fluoro-amodiaquine (FAQ) with Pyrimidines: Synthesis and Antimalarial Efficacy of FAQ-Pyrimidines.

Tripathi Mohit M   Taylor Dale D   Khan Shabana I SI   Tekwani Babu L BL   Ponnan Prija P   Das Ujjalkumar Subhash US   Velpandian Thirumurthy T   Rawat Diwan S DS  

ACS medicinal chemistry letters 20190313 5


To evade the possible toxicity associated with the formation of quinone-imine metabolite in amodiaquine (AQ), the <i>para</i>-hydroxyl group was replaced with a -F atom, and the resulting 4'-fluoro-amodiaquine (FAQ) was hybridized with substituted pyrimidines. The synthesized FAQ-pyrimidines displayed better <i>in vitro</i> potency than chloroquine (CQ) against the resistant <i>P. falciparum</i> strain (Dd2), exhibiting up to 47.3-fold better activity (IC<sub>50</sub>: 4.69 nM) than CQ (IC<sub>5  ...[more]

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