Background
For more than five decades, chloroquine (CQ) has been the main drug for the treatment of uncomplicated malaria in Mali. The emergence of
Unfortunately, the implementation of ACT among the most vulnerable populations living in highly malarious rural areas has been hampered by the limited availability and high cost of the new drugs. In Mali, the healthcare system operates on local cost-recovery, and current prices for ACT in public sector range from 700–1,500 CFA (US$1.50–4.0). Thus, the majority of patients did not have access to the newly recommended treatment and continued to use chloroquine despite its low efficacy. Therefore, there was a need to test other combination therapies already available in the country before ACT became more widely available. WHO recommendations allow for the use of non-artemisinin combination treatment regimens for the treatment of uncomplicated malaria in settings where the component drugs are efficacious and well tolerated. Data from several settings have demonstrated a similar efficacy between ACT and the combination of amodiaquine plus sulphadoxine-pyrimethamine (AQ+SP)
In Mali, SP is still efficacious (
Methods
Study site and population
The study was conducted in the rural village of Faladje, located 80 km Northwest of Bamako. The village has a Catholic mission health center that serves 23,000 inhabitants living in the village and surrounding areas. Malaria transmission is seasonal (July-October) with a peak in October. Most of the population is of the Bambara ethnic group with agriculture as the main occupation.
Study design and procedures
This was a randomized single-blind trial, conducted between July 2005 and January 2006, that included children between six and 59 months of age living in Faladje. After written informed consent of patients' parents or guardians, study subjects were enrolled if they fulfilled the following WHO
Treatment was administered according to body weight at the following doses: AQ: 10 mg/kg/day from day 0 to day 2; AS: 4 mg/kg/day from day 0 to day 2; SP: 25 mg/kg of sulphadoxine and 1.25 mg/kg of pyrimethamine in single dose on day 0. All drugs were administered directly by the study team and the child was observed for 30 minutes. If vomiting occurred before 30 minutes, the dose was repeated; for vomiting after 30 minutes, a half-dose was administered. In the case of persistent vomiting, the child was referred to a health center for rescue treatment with intramuscular or intravenous quinine and withdrawn from the study.
After the day of enrollment (day 0), the child was assessed on days 1, 2, 7, 14, and 28. Parents/guardians were encouraged to come to the clinic at any time when the child was sick.
Laboratory procedures
Capillary blood was obtained by fingerpick, thick and thin blood films were prepared and stained with 4% Giemsa for 20 minutes. Parasite densities were determined from thick blood smears by counting the number of asexual parasites per 300 WBCs assuming a WBC count of 7,500/μl. The same estimation method was used to calculate gametocyte density. Slides were read by an experienced medical microscopist, who was blinded to the treatment allocation. A negative blood film was defined as a slide with no parasites after review of 100 fields. Thin blood films were read only for parasite species determination. Ten percent of slides were read by a second reader, blinded to initial results. Discordant slides were read by a third microscopist.
Blood haemoglobin concentration was measured using a portable photometer (HemoCue: Anglholm, Sweden) on days 0, 14, 28 and any day of failure. Anaemia was defined as haemoglobin < 11.0 g/dl.
To distinguish recrudescence from new infection, molecular genotyping techniques were used for patients who failed after day 7. At enrollment and during the follow-up visits, blood spots were obtained on filter papers and evaluated at the Molecular Epidemiology and Drug Resistance Unit of the Malaria Research and Training Center in Bamako. Molecular analysis was done according to the following scheme: paired blots (from day 0 and the day of parasitaemia recurrence) were analysed by nested PCR of parasite merozoite surface proteins (MSP1 and MSP2) and microsatellite (CA1), to distinguish between new infection and recrudescence as previously described
Study endpoints classification
Treatment outcomes were classified following the 2003 WHO antimalarial drug efficacy guidelines
Ethical approval
The protocol was approved by the ethical committee of the University of Bamako Faculty of Medicine, Pharmacy, and Odonto-stomatology (FMPOS) and the Institutional Review Board of the United States Centers for Disease Control and Prevention before the study was started. Overall community and local authorities' permission were also obtained in addition to parent or guardian informed consent, according to procedures described earlier
Data entry and analysis
Data were double entered using Microsoft ACCESS and statistical analysis was performed using SPSS version 11.0 (Chicago, IL, USA). Baseline characteristics of subjects among groups were compared using the chi-square test for categorical variables and Mann-Whitney
Results
From July 2005 to January 2006, 876 children 6 to 59 months of age were screened for study entry (Figure
Baseline characteristics of children enrolled in antimalarial
Characteristics
AS+AQ N = 133
AS+SP N = 132
AQ+SP N = 132
Mean age ± S.D. (months)
34.49 ± 15.97
36.08 ± 15.97
37.56 ± 16.07
Range
6–59
6–59
8–59
Male gender, n (%)
72 (54.1)
64 (48.8)
82(62.1)
Mean weight ± SD (kg)
12.76 ± 3.30
12.77 ± 3.42
13.21 ± 3.49
Range
6.30–23.70
6–19.6
7.70–21.7
Mean height ± SD (cm)
92.05 ± 12.88
92.86 ± 14.18
94.39 ± 14.12
Range
63–115
64–120
65–133
Mean axillary temperature ± SD(°C)
38.59 ± .77
38.52 ± .78
38.58 ± .76
Range
37.5–40.2
37.5–40.6
37.5–40.8
Palpable spleen, n (%)
38(28.6)
40(30.3)
49 (37.1)
Mean haemoglobin ± SD (g/dl)
9.83 ± 1.80
9.71 ± 1.67
9.98 ± 1.59
Haemoglobin < 11 g/dl, n (%)
93(69.9)
102(77.3)
97(73.5)
GMPD/μl
24,113.4
22,846.8
24,051.7
Prior antimalarial use, n (%)
11(8.3)
4(3)
7(5.3)
Disease duration <= 1 day, n (%)
83(62.4)
92(69.7)
80(60.6)
Gametocyte carriage n (%)
1(0.8)
8 (6.1)
1(0.8)
AS+AQ, artesunate + amodiaquine; AS+SP, artesunate + sulphadoxine-pyrimethamine;
AQ+SP, amodiaquine + sulphadoxine-pyrimethamine. S.D, Standard deviation:
G/dl: Grams per deciliter
GMPD/μl: Geometric Mean Parasite Density per microliter.
P-values (not shown) were calculated from 2 × 3
Therapeutic efficacy of artesunate + amodiaquine, artesunate + sulphadoxine-pyrimethamine, and amodiaquine + sulphadoxine-pyrimethamine among children with uncomplicated malaria in Faladje, Mali
Characteristics
AS+AQ (N= 131)
AS+SP (N = 130)
AQ+SP (N = 130)
PCR uncorrected responses on day 28: n (%)
Failures
58 (44.3)
12 (9.2)
3(2.3)
ETF
0 (0)
2(1.5)
0(0)
LCF
14 (10.7)
2(1.5)
1(0.8)
LPF
44 (33.6)
8(6.2)
2(1.5)
*ACPR
73 (55.7)
118 (90.8)
127(97.7)
PCR corrected responses on day 28: n; %
Failures
6 (4.6)
4 (3.1)
1 (0.8)
ETF
0 (0)
2(1.6)
0(0)
LCF
2(1.5)
1(0.8)
0(0)
LPF
4(3.1)
1(0.8)
1 (0.8)
**ACPR
124(95.4)
125(96.9)
129(99.2)
AS+AQ, artesunate + amodiaquine; AS+SP, artesunate + sulphadoxine-pyrimethamine;
AQ+SP, amodiaquine + sulphadoxine-pyrimethamine
ETF, early treatment failure; LCF, late clinical failure; LPF, late parasitological failure; ACPR, adequate clinical and parasitological response.
Failures are the combination of ETF, LCF, and LPF. Percentages are rounded to achieve 100% of totals.
*
**
Profile of children screened, enrolled, and completing study protocol
Profile of children screened, enrolled, and completing study protocol.
At day 14, the proportion of children with anemia was significantly higher in AS+SP group (77.5%) when compared with AQ+SP (61.4%; p = 0.0046), but not with AS+AQ (65.9%; p = 0.030); the difference between the AS+AQ and AQ+SP groups was not statistically significant (Table
Haemoglobin concentration, anaemia, and parasitaemia among participants in an antimalarial
Characteristics
AS+AQ
AS+SP
AQ+SP
Day 0
N
133
132
132
Mean Haemoglobin ± S.D (g/dl)
9.83 ± 1.8
9.71 ± 1.59
9.98 ± 1.59
Anaemia (< 11 g/dl), n (%)
93 (69.9)
102 (77.3)
97 (73.5)
Day 14
N
131
130
130
§Mean Haemoglobin ± S.D (g/dl)
10.17 ± 1.5
9.89 ± 1.40
10.43 ± 1.49
*Anaemia (< 11 g/dl), n (%)
87 (65.9)
100 (77.5)
81 (61.4)
Day 28
N
105
127
130
§SMean Haemoglobin ± S.D (g/dl)
10.78 ± 1.49
10.5 ± 1.40
11.05 ± 1.52
**Anaemia (< 11 g/dl), n (%)
57(54.3)
76 (59.8)
60 (46.2)
Parasitaemia, n (%)
€Day2
14(10.5)
14(10.7)
67(50.7)
€Day3
2(1.5)
1(0.8)
8 (6.0)
Day14
5(3.8)
2(1.6)
2(1.5)
€Day28
31(29.5)
9(7.1)
3(2.3)
AS+AQ, artesunate + amodiaquine; AS+SP, artesunate + sulphadoxine-pyrimethamine; AQ+SP, amodiaquine + sulphadoxine-pyrimethamine
*
**
§Paired t-test comparison day 0 vs. day 14: overall, p < 0.01; AQ+SP, p = 0.001; AS+AQ, p = 0.011; AS+SP, p = 0.033.
§SPaired t-test comparison day 0 vs. day 28: overall, p < 0.001; AQ+SP, p < 0.001; AS+AQ, p < 0.001; AS+SP, p < 0.001
€
At day 28, the proportion of patients with anemia was 54.3%, 59.8%, and 46.2% in the AS+AQ, AS+SP, and AQ+SP groups respectively, but these differences were not statistically significant. Overall, the mean hemoglobin was significantly increased in all treatment groups at day 28 (10.78 ± 1.48 g/dl) when compared with day 0 (9.84 ± 1.68 g/dl) (p < 0.001); and the most significant increase was observed among children in AQ+SP (1.07 g/dl) group followed by AS+AQ (0.95 g/dl) and by AS+SP (0.79 g/dl) groups.
The proportion of patients with fever decreased from Day 0 (100%) to Day 1 (5.8%), Day 2 (2%), and Day 3 (1.5%) across all treatment arms. No difference was found among treatment groups at scheduled follow-up points with regard to the proportion of patients with fever. There were sharp declines in the proportion of children with parasitaemia from day 0 to day 2 in the AS+AQ (10.5%) and AS+SP (10.7%) groups, but not in AQ+SP (50.7%), (p < 0.001). By day 3, 1.5%, 0.8%, and 6% of patients were still parasitaemic in the AS+AQ, AS+SP, and AQ+SP groups respectively (p = 0.018) (Table
From day 0 to day 3, there was an increase of the proportion of gametocyte carriage followed by a decrease from day 3 to day 28 where that proportion approached zero. No statistical difference in gametocyte carriage between study arms was found at day 3 (p = 0.03) or day 28 (p = 0.16) (Figure
Proportion of children with gametocytes from day 0 to day 28, in Faladje among children aged 6–59 months
Proportion of children with gametocytes from day 0 to day 28, in Faladje among children aged 6–59 months.
Discussion
This study illustrated that the non-artemisinin containing combination AQ+SP was as efficacious as the artemisinin-based combinations AS+AQ and AS+SP for the treatment of uncomplicated
Children treated with AQ+SP had a lower prevalence of anaemia on days14 and 28 than children treated with AS+AQ or AS+SP. Anaemia prevalence appeared to track with parasitaemia prevalence, suggesting that the combination of two longer half-life drugs in AQ+SP may provide longer protection against new infections and subsequent anemia. While mean haemoglobin concentration on day 28 was higher among children treated with AQ+SP, this difference was not statistically significant. This is in consistent with prior studies, which have demonstrated similar mean haemoglobin concentration between AS+AQ and AQ+SP
The two artemisinin-based combinations, AS+AQ and AS+SP, showed faster parasite clearance than AQ+SP, but all three regimens resulted in prompt fever reduction. Despite the lower proportion of fever and parasitaemia observed during the first three days after treatment in the two ACT groups, there were more new infections in these groups than in the non-ACT group (AQ+SP). A greater risk of new infection following treatment with AS+AQ when compared with the AQ+SP has been reported earlier in low
Conclusion
The combination of AQ+SP provides a potentially low-cost alternative for treatment of uncomplicated
Competing interests
The authors declare that they have no competing interests.
Authors' contributions
In Mali, KK was the principal investigator and HM was the co-principal investigator of the study. At CDC, RN, MM, and AH contributed to the study design, protocol development, and manuscript writing. OY, HT, YK, EG, and RS participated in data collection, clinical investigation, and laboratory work. BT, AD were involved as field supervisors and laboratory data analysis. OD provided overall supervision in Mali. All authors participated in the writing and review of the final manuscript.