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Antimicrobial Agents and Chemotherapy, 08 1996, 1846-1854, Vol 40, No. 8
RG Ridley, W Hofheinz, H Matile, C Jaquet, A Dorn, R Masciadri, S Jolidon, WF Richter, A Guenzi, MA Girometta, H Urwyler, W Huber, S Thaithong and W Peters
We have synthesized several 4-aminoquinolines with shortened side chains
that retain activity against chloroquine-resistant isolates of Plasmodium
falciparum malaria (W. Hofheinz, C. Jaquet, and S. Jolidon, European patent
94116281.0, June 1995). We report here an assessment of the activities of
four selected compounds containing ethyl, propyl, and isopropyl side
chains. Reasonable in vitro activity (50% inhibitory concentration, <
100 nM) against chloroquine-resistant P. falciparum strains was
consistently observed, and the compounds performed well in a variety of
plasmodium berghei animal models. However, some potential drawbacks of
these compounds became evident upon in-depth testing. In vitro analysis of
more than 70 isolates of P. falciparum and studies with a mouse in vivo
model suggested a degree of cross-resistance with chloroquine. In addition,
pharmacokinetic analysis demonstrated the formation of N-dealkylated
metabolites of these compounds. These metabolites are similarly active
against chloroquine-susceptible strains but are much less active against
chloroquine-resistant strains. Thus, the clinical dosing required for these
compounds would probably be greater for chloroquine-resistant strains than
for chloroquine- susceptible strains. The clinical potential of these
compounds is discussed within the context of chloroquine's low therapeutic
ratio and toxicity.
Copyright © 1996 by the American Society for Microbiology. All rights reserved.
4-aminoquinoline analogs of chloroquine with shortened side chains retain activity against chloroquine-resistant Plasmodium falciparum
Pharma Division, F. Hoffmann-La Roche, Ltd., Basel, Switzerland. robert_g.ridley@roche.com
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