Abstract
BackgroundPrimaquine is the only licensed antimalarial for the radical cure of Plasmodium vivax infections. Many countries, however, do not administer primaquine due to fear of hemolysis in those with glucose-6-phosphate dehydrogenase (G6PD) deficiency. In other settings, primaquine is given without G6PD testing, putting patients at risk of hemolysis. New rapid diagnostic tests (RDTs) offer the opportunity to screen for G6PD deficiency prior to treatment with primaquine. Here we assessed the cost-effectiveness of using G6PD RDTs on the Thailand-Myanmar border and provide the model as an online tool for use in other settings.Methods/Principal findingsDecision tree models for the management of P. vivax malaria evaluated the costs and disability-adjusted life-years (DALYs) associated with recurrences and primaquine-induced hemolysis from a health care provider perspective. Screening with G6PD RDTs before primaquine use was compared to (1) giving chloroquine alone and (2) giving primaquine without screening. Data were taken from a recent study on the impact of primaquine on P. vivax recurrences and a literature review. Compared to the use of chloroquine alone, the screening strategy had similar costs while averting 0.026 and 0.024 DALYs per primary infection in males and females respectively. Compared to primaquine administered without screening, the screening strategy provided modest cost savings while averting 0.011 and 0.004 DALYs in males and females respectively. The probabilistic sensitivity analyses resulted in a greater than 75% certainty that the screening strategy was cost-effective at a willingness to pay threshold of US$500, which is well below the common benchmark of per capita gross domestic product for Myanmar.Conclusions/SignificanceIn this setting G6PD RDTs could avert DALYs by reducing recurrences and reducing hemolytic risk in G6PD deficient patients at low costs or cost savings. The model results are limited by the paucity of data available in the literature for some parameter values, including the mortality rates for both primaquine-induced hemolysis and P. vivax. The online model provides an opportunity to use different parameter estimates to examine the validity of these findings in other settings.
Highlights
Plasmodium vivax is an important public health concern, in Asia and South America, where it is responsible for the majority of malaria cases
Primaquine is given without testing for glucose-6-phosphate dehydrogenase (G6PD) deficiency, putting patients at risk of potentially fatal hemolysis
New rapid diagnostic tests provide the opportunity to screen for G6PD deficiency prior to giving patients primaquine
Summary
Plasmodium vivax is an important public health concern, in Asia and South America, where it is responsible for the majority of malaria cases. A single infection of P. vivax can lead to multiple relapses due to its ability to form dormant liver stage parasites called hypnozoites. These relapses are indistinguishable from new infections and repeated episodes can lead to a cumulative risk of anemia and malnutrition [5, 6]. In short latency relapse settings, the majority of P. vivax cases are thought to be due to relapses [7]. Primaquine is given without G6PD testing, putting patients at risk of hemolysis. New rapid diagnostic tests (RDTs) offer the opportunity to screen for G6PD deficiency prior to treatment with primaquine. We assessed the cost-effectiveness of using G6PD RDTs on the Thailand-Myanmar border and provide the model as an online tool for use in other settings
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