Clinical and parasitological response to oral chloroquine and primaquine in uncomplicated human Plasmodium knowlesi infections
Background: Plasmodium knowlesi is a cause of symptomatic and potentially fatal infections in humans. There are no studies assessing the detailed parasitological response to treatment of knowlesi malaria infections in man and whether antimalarial resistance occurs. Methods: A prospective observa...
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my.unimas.ir.158082021-04-30T14:12:50Z http://ir.unimas.my/id/eprint/15808/ Clinical and parasitological response to oral chloroquine and primaquine in uncomplicated human Plasmodium knowlesi infections Daneshvar, C. Davis, T.M.E Cox-Singh, J. Mohammad Zakri, Rafa’ee Siti Khatijah, Binti Zakaria Paul C, Divis Balbir, Singh RA Public aspects of medicine Background: Plasmodium knowlesi is a cause of symptomatic and potentially fatal infections in humans. There are no studies assessing the detailed parasitological response to treatment of knowlesi malaria infections in man and whether antimalarial resistance occurs. Methods: A prospective observational study of oral chloroquine and primaquine therapy was conducted in consecutive patients admitted to Kapit Hospital, Sarawak, Malaysian Borneo with PCR-confirmed single P. knowlesi infections. These patients were given oral chloroquine for three days, and at 24 hours oral primaquine was administered for two consecutive days, primarily as a gametocidal agent. Clinical and parasitological responses were recorded at 6-hourly intervals during the first 24 hours, daily until discharge and then weekly to day 28. Vivax malaria patients were studied as a comparator group. Results: Of 96 knowlesi malaria patients who met the study criteria, 73 were recruited to an assessment of the acute response to treatment and 60 completed follow-up over 28 days. On admission, the mean parasite stage distributions were 49.5%, 41.5%, 4.0% and 5.6% for early trophozoites, late trophozoites, schizonts and gametocytes respectively. The median fever clearance time was 26.5 [inter-quartile range 16-34] hours. The mean times to 50% (PCT50) and 90% (PCT90) parasite clearance were 3.1 (95% confidence intervals [CI] 2.8-3.4) hours and 10.3 (9.4-11.4) hours. These were more rapid than in a group of 23 patients with vivax malaria 6.3 (5.3-7.8) hours and 20.9 (17.6- 25.9) hours; P = 0.02). It was difficult to assess the effect of primaquine on P. knowlesi parasites, due to the rapid anti-malarial properties of chloroquine and since primaquine was administered 24 hours after chloroquine. No P. knowlesi recrudescences or re-infections were detected by PCR. Conclusions: Chloroquine plus primaqine is an inexpensive and highly effective treatment for uncomplicated knowlesi malaria infections in humans and there is no evidence of drug resistance. Further studies using alternative anti-malarial drugs, including artemisinin derivatives, would be desirable to define optimal management strategies for P. knowlesi. BioMed Central Ltd. 2010 Article PeerReviewed text en http://ir.unimas.my/id/eprint/15808/7/Clinicalandparasitological.pdf Daneshvar, C. and Davis, T.M.E and Cox-Singh, J. and Mohammad Zakri, Rafa’ee and Siti Khatijah, Binti Zakaria and Paul C, Divis and Balbir, Singh (2010) Clinical and parasitological response to oral chloroquine and primaquine in uncomplicated human Plasmodium knowlesi infections. Malaria Journal, 9 (238). ISSN 14752875 https://malariajournal.biomedcentral.com/articles/10.1186/1475-2875-9-238 DOI: 10.1186/1475-2875-9-238 |
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RA Public aspects of medicine Daneshvar, C. Davis, T.M.E Cox-Singh, J. Mohammad Zakri, Rafa’ee Siti Khatijah, Binti Zakaria Paul C, Divis Balbir, Singh Clinical and parasitological response to oral chloroquine and primaquine in uncomplicated human Plasmodium knowlesi infections |
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Background: Plasmodium knowlesi is a cause of symptomatic and potentially fatal infections in humans. There are
no studies assessing the detailed parasitological response to treatment of knowlesi malaria infections in man and whether antimalarial resistance occurs.
Methods: A prospective observational study of oral chloroquine and primaquine therapy was conducted in
consecutive patients admitted to Kapit Hospital, Sarawak, Malaysian Borneo with PCR-confirmed single P. knowlesi
infections. These patients were given oral chloroquine for three days, and at 24 hours oral primaquine was
administered for two consecutive days, primarily as a gametocidal agent. Clinical and parasitological responses
were recorded at 6-hourly intervals during the first 24 hours, daily until discharge and then weekly to day 28. Vivax malaria patients were studied as a comparator group.
Results: Of 96 knowlesi malaria patients who met the study criteria, 73 were recruited to an assessment of the
acute response to treatment and 60 completed follow-up over 28 days. On admission, the mean parasite stage
distributions were 49.5%, 41.5%, 4.0% and 5.6% for early trophozoites, late trophozoites, schizonts and gametocytes
respectively. The median fever clearance time was 26.5 [inter-quartile range 16-34] hours. The mean times to 50%
(PCT50) and 90% (PCT90) parasite clearance were 3.1 (95% confidence intervals [CI] 2.8-3.4) hours and 10.3 (9.4-11.4)
hours. These were more rapid than in a group of 23 patients with vivax malaria 6.3 (5.3-7.8) hours and 20.9 (17.6-
25.9) hours; P = 0.02). It was difficult to assess the effect of primaquine on P. knowlesi parasites, due to the rapid
anti-malarial properties of chloroquine and since primaquine was administered 24 hours after chloroquine. No
P. knowlesi recrudescences or re-infections were detected by PCR.
Conclusions: Chloroquine plus primaqine is an inexpensive and highly effective treatment for uncomplicated
knowlesi malaria infections in humans and there is no evidence of drug resistance. Further studies using alternative anti-malarial drugs, including artemisinin derivatives, would be desirable to define optimal management strategies for P. knowlesi. |
format |
Article |
author |
Daneshvar, C. Davis, T.M.E Cox-Singh, J. Mohammad Zakri, Rafa’ee Siti Khatijah, Binti Zakaria Paul C, Divis Balbir, Singh |
author_facet |
Daneshvar, C. Davis, T.M.E Cox-Singh, J. Mohammad Zakri, Rafa’ee Siti Khatijah, Binti Zakaria Paul C, Divis Balbir, Singh |
author_sort |
Daneshvar, C. |
title |
Clinical and parasitological response to oral chloroquine and primaquine in uncomplicated human Plasmodium knowlesi infections |
title_short |
Clinical and parasitological response to oral chloroquine and primaquine in uncomplicated human Plasmodium knowlesi infections |
title_full |
Clinical and parasitological response to oral chloroquine and primaquine in uncomplicated human Plasmodium knowlesi infections |
title_fullStr |
Clinical and parasitological response to oral chloroquine and primaquine in uncomplicated human Plasmodium knowlesi infections |
title_full_unstemmed |
Clinical and parasitological response to oral chloroquine and primaquine in uncomplicated human Plasmodium knowlesi infections |
title_sort |
clinical and parasitological response to oral chloroquine and primaquine in uncomplicated human plasmodium knowlesi infections |
publisher |
BioMed Central Ltd. |
publishDate |
2010 |
url |
http://ir.unimas.my/id/eprint/15808/7/Clinicalandparasitological.pdf http://ir.unimas.my/id/eprint/15808/ https://malariajournal.biomedcentral.com/articles/10.1186/1475-2875-9-238 |
_version_ |
1698700768190660608 |