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In VivoandIn VitroEfficacy of Chloroquine againstPlasmodium malariaeandP. ovalein Papua, Indonesia

Siswantoro H., Russell B., Ratcliff A., Prasetyorini B., Chalfein F., Marfurt J., Kenangalem E., Wuwung M., Piera KA., Ebsworth EP., Anstey NM., Tjitra E., Price RN.

<jats:title>ABSTRACT</jats:title><jats:p>Reports of potential drug-resistant strains of<jats:italic>Plasmodium malariae</jats:italic>in western Indonesia raise concerns that chloroquine resistance may be emerging in<jats:italic>P. malariae</jats:italic>and<jats:italic>P. ovale</jats:italic>. In order to assess this,<jats:italic>in vivo</jats:italic>and<jats:italic>in vitro</jats:italic>efficacy studies were conducted in patients with monoinfection in Papua, Indonesia. Consecutive patients with uncomplicated malaria due to<jats:italic>P. ovale</jats:italic>or<jats:italic>P. malariae</jats:italic>were enrolled in a prospective clinical trial, provided with supervised chloroquine treatment, and followed for 28 days. Blood from patients with<jats:italic>P. malariae</jats:italic>or<jats:italic>P. ovale</jats:italic>parasitemia greater than 1,000 per microliter underwent<jats:italic>in vitro</jats:italic>antimalarial drug susceptibility testing using a modified schizont maturation assay. Of the 57 evaluable patients in the clinical study (<jats:italic>P. malariae</jats:italic>,<jats:italic>n</jats:italic>= 46;<jats:italic>P. ovale</jats:italic>,<jats:italic>n</jats:italic>= 11), none had recurrence with the same species during follow-up. The mean parasite reduction ratio at 48 h was 86 (95% confidence interval [CI], 57 to 114) for<jats:italic>P. malariae</jats:italic>and 150 (95% CI, 54 to 245) for<jats:italic>P. ovale</jats:italic>(<jats:italic>P</jats:italic>= 0.18). One patient infected with<jats:italic>P. malariae</jats:italic>, with 93% of parasites at the trophozoite stage, was still parasitemic on day 4.<jats:italic>In vitro</jats:italic>drug susceptibility assays were carried out successfully for 40 isolates (34 infected with<jats:italic>P. malariae</jats:italic>and 6 with<jats:italic>P. ovale</jats:italic>). The<jats:italic>P. malariae</jats:italic>infections at trophozoite stages had significantly higher chloroquine 50% effective concentrations (EC<jats:sub>50</jats:sub>s) (median, 127.9 nM [range, 7.9 to 2,980]) than those initially exposed at the ring stage (median, 14.0 nM [range, 3.5 to 27.0];<jats:italic>P</jats:italic>= 0.01). The EC<jats:sub>50</jats:sub>for chloroquine in<jats:italic>P. ovale</jats:italic>was also higher in an isolate initially at the trophozoite stage (23.2 nM) than in the three isolates predominantly at ring stage (7.8 nM). Chloroquine retains adequate efficacy against<jats:italic>P. ovale</jats:italic>and<jats:italic>P. malariae</jats:italic>, but its marked stage specificity of action may account for reports of delayed parasite clearance times.</jats:p>

Original publication

DOI

10.1128/aac.01122-10

Type

Journal article

Journal

Antimicrobial Agents and Chemotherapy

Publisher

American Society for Microbiology

Publication Date

01/2011

Volume

55

Pages

197 - 202