Efficacy of atovaquone against Babesia gibsoni in vivo and in vitro

The therapeutic efficacy of atovaquone against Babesia gibsoni was examined in three dogs experimentally infected with B. gibsoni isolated from naturally infected dogs in Aomori Prefecture, Japan. Once parasitemia reached 10%, atovaquone was administered orally (30 mg/kg twice daily for 7 days). Wit...

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Published in:Veterinary parasitology 2004-09, Vol.124 (1), p.9-18
Main Authors: Matsuu, Aya, Koshida, Yushi, Kawahara, Megumi, Inoue, Kenichi, Ikadai, Hiromi, Hikasa, Yoshiaki, Okano, Shozo, Higuchi, Seiichi
Format: Article
Language:English
Subjects:
1, 4-hydroxynaphthoquinone
Administration, Oral
Animals
antiprotozoal agents
Antiprotozoal Agents - pharmacology
Antiprotozoal Agents - therapeutic use
Atovaquone
Babesia - drug effects
Babesia gibsoni
babesiosis
Babesiosis - drug therapy
Babesiosis - veterinary
Canine babesiosis
Chemotherapy
Dog Diseases - drug therapy
Dogs
dose response
Dose-Response Relationship, Drug
drug efficacy
drug evaluation
Drug Resistance
drug therapy
Female
in vitro studies
in vivo studies
naphthoquinones
Naphthoquinones - pharmacology
Naphthoquinones - therapeutic use
parasitemia
Parasitic Sensitivity Tests - veterinary
Thrombocytopenia
Thrombocytopenia - parasitology
Thrombocytopenia - veterinary
Treatment Outcome
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Summary:The therapeutic efficacy of atovaquone against Babesia gibsoni was examined in three dogs experimentally infected with B. gibsoni isolated from naturally infected dogs in Aomori Prefecture, Japan. Once parasitemia reached 10%, atovaquone was administered orally (30 mg/kg twice daily for 7 days). Within 2 days of atovaquone treatment, the parasite disappeared from blood smears without any clinical side effects. Anemia and thrombocytopenia were significantly improved in all the dogs. However, a polymerase chain reaction assay revealed that a B. gibsoni marker gene was intermittently present in peripheral blood after atovaquone therapy, indicating that the organism had not been eliminated, and parasites reappeared in blood smears 33 days after the last treatment. To investigate the change in sensitivity against atovaquone, an in vitro sensitivity test was performed using peripheral blood obtained from an untreated dog that was infected with the original parasite isolate, and from two of the experimentally infected and atovaquone-treated animals (blood was collected at the time of the post-treatment recurrence of the B. gibsoni infection). Atovaquone was added to the culture medium to final concentrations of 0.1, 1, 10, 100, and 1000 nM. For the untreated parasites, complete growth inhibition occurred at 1000 nM of atovaquone, whereas the recurrent parasites were inhibited by only 39.52 ± 8.34% and 31.31 ± 8.14% at this concentration after 48 h of incubation. Thus, the recurring parasites were less sensitive to atovaquone than the untreated originally isolated parasites.
ISSN:0304-4017
1873-2550
DOI:10.1016/j.vetpar.2004.07.005