Malaria Clinical Trial
Official title:
Parasite-based Diagnosis for Malaria in Uganda: Feasibility and Cost-Effectiveness
The purpose of this study is to compare the cost-effectiveness of treating malaria based on three methods of diagnosis (rapid test, microscopy and presumptive diagnosis) among patients attending level three government health centres located in areas of low and high transmission intensities in Uganda. The study hypotheses are: in both low and high transmission areas, cost-effectiveness of malaria treatment with Artemether-Lumefantrine will be improved by the adoption of rapid diagnostic tests when compared with presumptive diagnosis or microscopy; and the difference between the cost-effectiveness of Artemether-Lumefantrine treatment following rapid diagnostic test or microscopy versus presumptive diagnosis will be greatest in low transmission areas.
The development of drug resistance in malaria parasites lead the Uganda Ministry of Health
(MoH) to change the first-line anti-malarial treatment from the cheap
Chloroquine/Sulfadoxine-Pyrimethamine combination to a more expensive
Artemether-Lumefantrine. The MoH recommends treatment of all fever cases as malaria within
24 hours of illness with first-line drug. Under this policy, patients who do not have
malaria but present with febrile illness will receive Coartem® resulting in significant drug
wastage. With the increased cost of first-line drugs, this wastage places a substantial and
potentially remediable burden on the health budget. As such, there is a need to gauge
whether more accurate malaria diagnosis through microscopy and/or rapid diagnostic tests,
might improve the cost-effectiveness of the new treatment regimes.
Specific objectives
1. To assess the feasibility of rapid test and microscopy in diagnosis of malaria at
health centre III.
2. To compare the cost-effectiveness of treating malaria with Artemether- Lumefantrine
based on microscopy, rapid test and presumptive diagnosis in different transmission
intensities
3. To assess whether introduction of malaria parasite-based diagnosis (rapid test or
microscopy) at government Health Centre III improves the overall cost-effectiveness of
outpatient management of febrile illness
Sample size determination The sample size was determined using standard formula. Estimating
the sensitivity of either test to be 90%, Zα =1.96 and after stratifying for age (<5 years
and ≥5 years), the calculated sample is 272 per health centre. Therefore, the total number
of patients for 6 health centres in two districts = 6 x 272 = 1632.
Baseline: Baseline data was collected on the current malaria treatment practices;
clinicians' view of malaria diagnosis; concerns towards the new treatment; and health centre
staffing. Geographical locations of all visited government health centres was recorded using
Germin etrex global positioning system (Germin International Inc., Olathe, USA). At six
selected health centres, social and demographic data was collected from 613 patients.
Implementation of intervention: The main intervention is comprised of three malaria
diagnostic approaches: presumptive diagnosis, field microscopy and rapid test (Paracheck Pf®
device - Orchid Biomedical Systems, Goa, India). Each of these approaches was randomly
allocated to a health centre. The first-line drug used is Artemether/Lumefantrine
(20mg/120mg) (Novartis, Switzerland).
Consenting subjects are consecutively enrolled at the point when the attending clinician
suspects that they have uncomplicated malaria. Where microscopy is the main diagnostic
method, thick and thin blood smears are prepared per patient enrolled. Where rapid test is
the main method, all patients are tested. One hundred patients per health centre are
randomly selected to provide blood specimens for validation using expert microscopy and PCR
as "gold standard." After enrolment, patients are systematically tracked until departure
from the health centre. Patients are followed up on the seventh day of treatment to assess
their clinical improvement. Those who fail to return on the scheduled date are traced from
their homes on the eighth day.
Follow-up activities include: documentation of drugs prescribed and or dispensed; clinically
assess the patient's status in comparison to Day 0; perform further tests including PCR if
the patient does not show improvement; pill counting of drugs remaining - if the patient has
not completed the dose; documentation of reasons for not completing dose; and documentation
if the patient bought the prescribed drugs that were out of stock on Day 0.
Effectiveness is measured as the number of patients commencing treatment with
Artemether/Lumefantrine. However, patients are followed up and effectiveness also measured
on the 7th day of treatment indicated by their clinical improvement. The feasibility of the
diagnostic methods is ongoing from the March 2010 to date.
;
Allocation: Non-Randomized, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Diagnostic
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