Data from Brazil (most of which were from Amazonia and a few from French Guiana) have identified P vivax relapse rates of 39.6% after primaquine regimens (total doses ranging from 2.2 to 4.9 mg/kg), half of which occurred
within 108 days of radical cure[10]; the study advocates that the primaquine total dose above which this website relapses do not occur is 3.6 mg/kg. The failure rate of the 30 mg/day regimen in the present study (roughly 30%) is not so different from those observed by Pedro and colleagues[10] but higher than the other data found in the literature (efficacy of 95%).[4] However, all three relapsing patients were prescribed primaquine total doses of above 3.6 mg/kg, which seems contradictory to the findings in Brazil,[10] and would suggest that some strains from French Guiana need higher primaquine doses, closer to the Chesson type of P vivax. More data from records of travelers who acquired
P vivax in French Guiana would be required to discern whether the high risk of relapse observed after standard radical cure on a small sample of records reflects the current risk of relapse in this area. If selleck chemicals so, efficacy of potentially more effective alternative regimens should be comparatively assessed. The fact that two of the patients who relapsed had body weight >70 kg (100 and 105 kg) may have played a role as the initial regimen for them was 0.3 mg/kg daily whereas the second one was 0.5 mg/kg daily. On the basis of a trend of higher risk of relapse after standard radical cure in high body weight Olopatadine patients with P vivax infections, Baird and colleagues[6] advocated for a regimen of 0.5 mg/kg primaquine daily for 14 days for patients weighing more than 70 kg. This recommendation has since been partially integrated
by the CDC experts meeting: although the standard recommended course is still 30 mg/day over 14 days, it is now specified that for individuals weighing more than 70 kg, the treatment could be extended to provide a total dose of 6 mg/kg.[3] In our case series, radical cure of P ovale and P vivax infections used primaquine alone; however, as higher efficiency of primaquine was demonstrated when given concurrently with blood schizonticides,[4] an alternative could be to give a combinative treatment as first-line radical cure. Relapses of P vivax infections from French Guiana were frequently observed in our experience of radical cure with primaquine at 30 mg daily. More data are needed to estimate properly the relapse rate of P vivax infections from French Guiana after primaquine radical cure and further comparative studies would be required to test suitably the hypothesis that radical cure dosage could be adapted to body weight in order to reduce the risk of relapse in this population. The authors state they have no conflicts of interest to declare.