Abstract
BackgroundSickle cell disease (SCD) is a genetic disorder common in malaria endemic areas. In endemic areas, malaria is a major cause of morbidity and mortality among SCD patients. This suggests the need for prompt initiation of efficacious anti-malarial therapy in SCD patients with acute malaria. However, there is no information to date, on the efficacy or safety of artemisinin combination therapy when used for malaria treatment in SCD patients.MethodsChildren with SCD and acute uncomplicated malaria (n = 60) were randomized to treatment with artesunate-amodiaquine (AA), or artemether-lumefantrine (AL). A comparison group of non-SCD children (HbAA genotype; n = 59) with uncomplicated malaria were also randomized to treatment with AA or AL. Recruited children were followed up and selected investigations were done on days 1, 2, 3, 7, 14, 28, 35, and 42. Selected clinical and laboratory parameters of the SCD patients were also compared with a group of malaria-negative SCD children (n = 82) in steady state.ResultsThe parasite densities on admission were significantly lower in the SCD group, compared with the non-SCD group (p = 0.0006). The parasite reduction ratio (PRR) was lower, clearance was slower (p < 0.0001), and time for initial parasitaemia to decline by 50 and 90% were longer for the SCD group. Adequate clinical and parasitological response (ACPR) on day 28 was 98.3% (58/59) in the SCD group and 100% (57/57) in the non-SCD group. Corresponding ACPR rates on day 42 were 96.5% (55/57) in the SCD group and 96.4% (53/55) in the non-SCD group. The fractional changes in haemoglobin, platelets and white blood cell counts between baseline (day 0) and endpoint (day 42) were 16.9, 40.6 and 92.3%, respectively, for the SCD group, and, 12.3, 48.8 and 7.5%, respectively, for the non-SCD group. There were no differences in these indices between AA- and AL-treated subjects.ConclusionsThe parasite clearance of SCD children with uncomplicated malaria was slower compared with non-SCD children. AA and AL showed similar clinical and parasitological effects in the SCD and non-SCD groups. The alterations in WBC and platelet counts may have implications for SCD severity.Trial registrationCurrent controlled trials ISRCTN96891086.
Highlights
Sickle cell disease (SCD) is a genetic disorder common in malaria endemic areas
Study site The study was conducted at the Outpatients Department (OPD) and Paediatric Sickle Cell Clinic of the Department of Child Health (DCH), Korle Bu Teaching Hospital (KBTH), between January 2010 and December 2011
Baseline characteristics A total of 648 SCD children presenting with acute febrile illness at the OPD and Paediatric Sickle Cell Clinic, DCH, were screened for inclusion
Summary
Malaria is a major cause of morbidity and mortality among SCD patients. This suggests the need for prompt initiation of efficacious anti-malarial therapy in SCD patients with acute malaria. Even though evidence from recent studies indicates that overall prevalence of malaria in SCD subjects is comparatively low, it has been shown that among hospitalized SCD patients mortality is higher among those with malaria compared with those without [9,10,11,12,13,14] These considerations suggest that prompt initiation of efficacious anti-malarial therapy among acutely ill SCD patients with confirmed malaria is important. There is paucity of information on the effects of antimalarial treatment in SCD patients with acute malaria in general, and no report to date on the efficacy or safety of currently recommended first-line malaria treatments, artemisinin combination therapy (ACT), when used for treatment in SCD patients with malaria
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