Dihydroquinazolinone Inhibitors of Proliferation of Blood and Liver Stage Malaria Parasites
Author(s) -
Emily R. Derbyshire,
Jaeki Min,
W. Armand Guiguemde,
Julie Clark,
Michele Connelly,
Andreia D. Magalhães,
R. Kiplin Guy,
Jon Clardy
Publication year - 2013
Publication title -
antimicrobial agents and chemotherapy
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.07
H-Index - 259
eISSN - 1070-6283
pISSN - 0066-4804
DOI - 10.1128/aac.02148-13
Subject(s) - plasmodium berghei , malaria , pharmacology , plasmodium falciparum , moiety , toxicity , biology , potency , antimalarial agent , immunology , biochemistry , chemistry , in vitro , stereochemistry , medicine
Drugs that target both the liver and blood stages of malaria will be needed to reduce the disease's substantial worldwide morbidity and mortality. Evaluation of a 259-member library of compounds that block proliferation of the blood stage of malaria revealed several scaffolds—dihydroquinazolinones, phenyldiazenylpyridines, piperazinyl methyl quinolones, and bis-benzimidazoles—with promising activity against the liver stage. Focused structure-activity studies on the dihydroquinazolinone scaffold revealed several molecules with excellent potency against both blood and liver stages. One promising early lead with dual activity is 2-(p -bromophenyl)-3-(2-(diethylamino)ethyl)-2,3-dihydroquinazolin-4(1H )-one with 50% effective concentrations (EC50 s) of 0.46 μM and 0.34 μM against liver stagePlasmodium berghei ANKA and blood stagePlasmodium falciparum 3D7 parasites, respectively. Structure-activity relationships revealed that liver stage activity for this compound class requires a 3-dialkyl amino ethyl group and is abolished by substitution at theortho -position of the phenyl moiety. These compounds have minimal toxicity to mammalian cells and are thus attractive compounds for further development.
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