Double blind randomised clinical trial of two different regimens of oral artesunate in falciparum malaria.

A double blind randomized comparative trial of the efficacy of 7-day and 5-day courses of oral artesunate at 600 mg was studied in 89 Thai patients with uncomplicated falciparum malaria. Eighty patients completed the 28-day follow-up period. Artesunate was found to be well tolerated in either regimen. There was an increase of 7% in the cure rate obtained from a 7-day regimen. In 43 patients with a 7-day regimen, the cure rate was 92.5% and 15 patients showed P. vivax in their peripheral blood between days 12 and 34. The mean fever and parasite clearance times were 20 and 40 hours, respectively. In 46 patients with a 5-day regimen, the cure rate was 85% and 8 patients showed P. vivax during days 13 and 24. The mean fever and parasite clearance times were 29 and 40 hours, respectively. Although the cure rates of oral artesunate were high in both regimens, the efficacy was considered unsatisfactory since the aim of the treatment is to achieve 100% cure rate. We suggest however that the extension of the duration of treatment to 7 days together with the increase in total dose may improve therapeutic efficacy of artesunate in falciparum malaria.

[1]  S. Looareesuwan,et al.  Double blind randomised clinical trial of oral artesunate at once or twice daily dose in falciparum malaria. , 1991, The Southeast Asian journal of tropical medicine and public health.

[2]  R. Ekong,et al.  Synergism between arteether and mefloquine or quinine in a multidrug-resistant strain of Plasmodium falciparum in vitro. , 1990, Transactions of the Royal Society of Tropical Medicine and Hygiene.

[3]  D. Warhurst,et al.  The effect of combinations of qinghaosu (artemisinin) with standard antimalarial drugs in the suppressive treatment of malaria in mice. , 1987, Transactions of the Royal Society of Tropical Medicine and Hygiene.

[4]  T. Harinasuta,et al.  Quinine and quinidine in malaria in Thailand. , 1987, Acta Leidensia.

[5]  W. Wernsdorfer,et al.  A phase-III clinical trial of mefloquine in children with chloroquine-resistant falciparum malaria in Thailand. , 1987, Bulletin of the World Health Organization.

[6]  W. Wernsdorfer,et al.  Mefloquine, sulfadoxine, and pyrimethamine in the treatment of symptomatic falciparum malaria: a double-blind trial for determining the most effective dose. , 1987, Bulletin of the World Health Organization.

[7]  Pe Than Myint,et al.  The efficacy of artemether (qinghaosu) in Plasmodium falciparum and P. vivax in Burma. , 1986, The Southeast Asian journal of tropical medicine and public health.

[8]  W. Wernsdorfer,et al.  A phase II clinical trial of mefloquine in patients with chloroquine-resistant falciparum malaria in Thailand. , 1983, Bulletin of the World Health Organization.

[9]  Guoqiao Li,et al.  ANTIMALARIAL ACTIVITY OF MEFLOQUINE AND QINGHAOSU , 1982, The Lancet.

[10]  Liu Gq Clinical study on the use of artemether in treating pernicious malaria , 1982 .

[11]  T. Chongsuphajaisiddhi,et al.  In vivo and in vitro sensitivity of Falciparum malaria to quinine in Thai children. , 1981, Annals of tropical paediatrics.

[12]  L. Sax,et al.  DRUG SENSITIVITY OF PLASMODIUM FALCIPARUM An In-vitro Microtechnique , 1978, The Lancet.