Malaria Clinical Trial
Official title:
Comparison of Safety, Tolerability and Efficacy of Three Drug Combinations for Intermittent Preventive Treatment in Children Aged 1-5 Years in an Area of Seasonal Malaria Transmission in Upper River Division, The Gambia
Intermittent preventive treatment (IPT) offers a way of preventing malaria infection without compromising the development of malaria immunity or encouraging drug resistance. The effect of IPT in children in the prevention of malaria has been evaluated in a number of trials in areas of seasonal malaria transmission. Results from these trials have shown that IPTc provided between 40% - 86% protection against clinical malaria. In 2006, a trial that compared two methods of IPTc delivery was carried out in Upper River Division, The Gambia. Preliminary results of the trial have shown that the treatment was very effective as only 4% (45/1133) of the children seen at the end of year cross-sectional survey were parasitaemic. Tolerability was assessed in a subset of 1100 children and the results showed that about 13.5% of children developed mild to moderate vomiting. Malaise was present in about 10% of the study subjects. Severe adverse events were rare. Thus it is important to investigate if other drug regimens might be equally effective in preventing malaria but less likely to cause adverse events. During the 2007 malaria transmission season, 1009 children aged 1-5 years will be individually randomized to receive amodiaquine plus SP, piperaquine plus SP or Artekin TM (dihdroartemisinin plus piperaquine) at monthly intervals on three occasions during the months of September, October, and November. To determine the prevalence of side effects following drug administration participants in each treatment group will be visited at home three and seven days after each round of drug administration and a side effects questionnaire completed. To help establish whether these adverse events are drug related, the same questionnaire will be administered after each treatment round, to 286 age-matched children who are not part of the trial. The primary ends points will be the incidence of adverse events.
Objectives
Primary Objective To determine the safety and tolerability of amodiaquine(AQ) (three days)
plus sulfadoxine-pyrimethamine(SP) (one day), piperaquine(PQP) (three days) plus SP (one
day), and Artekin TM (PQP plus dihydroartemisinin, DHA) (3 days) when used for seasonal IPT
in children.
Secondary Objective To determine the efficacy of AQ (three days) plus SP (one day), PQP
(three days) plus SP (one day) and Artekin TM (3 days) when used for seasonal IPT in
children.
3.4 Randomisation Open-label, individual randomisation was carried out three weeks before
the first dose of IPTc administration in September 2007. Study subjects were individually
randomised into either the AQ plus SP, PQP plus SP or ArtekinTM treatment groups in a 1:1:1
fashion. An independent statistician generated the randomizing subject study number (SSN)
that assigned each SSN to one of the treatment groups. A photo ID card was given to all
participants to facilitate identification at every contact, at home or in the health
centres.
3.5 Drug distribution at the health centres Study subjects and their parents were informed
about the date of treatment approximately one week before any intervention. Treatment is
scheduled to be given during the months of September, October and November. Drugs are to be
given at the nearest health centre by a designated member of staff. Tablets are crushed,
mixed with honey or suspended in water and given on a spoon. Staff who administer drugs at
the health centre play no further part in the trial. All participants are kept under
observation for 30 minutes after drugs are taken. In case of vomiting, the drug is
re-administrated. At the time of each monthly drug administration, a brief clinical
assessment is carried out. Children who are febrile are screened for malaria using a rapid
antigen test. Children found to have malaria are treated with Lumefantrine-artemether
(CoartemTM, Norvatis Pharma., Basel Switzerland).
3.7 Morbidity surveillance during the rainy season Passive surveillance for malaria will be
maintained throughout the transmission season. Parents/guardians are being encouraged to
take their children to the health centre identified as being closest to their home at any
time that their child becomes unwell. Project staff are based at each of these health
facilities to identify children in the trial and to ensure that they are seen, properly
investigated and treated promptly. At each clinic visit, axillary temperature is recorded
using a digital thermometer and haemoglobin concentration measured using a Hemocue machine.
A dipstick for diagnosis of malaria is to be used if fever (axillary temperature of ³
37.5°C) or a history of fever within the previous 48 hours is present. In such cases, a
thick blood smear is also be collected for subsequent confirmation of the diagnosis. Study
subjects with documented fever (axillary temperature of ³ 37.5°C) or history of recent fever
and malaria parasitaemia are treated with Coartem. The treatment of study subjects seen at
the health centres for other conditions is being carried out in accordance with national
guidelines.
3.8 End of malaria transmission season cross-sectional survey Children enrolled in the study
will be seen at the OPD clinic at the end of malaria transmission season for examination by
a study physician and a finger-prick blood sample will be obtained for preparation of a
thick blood smear and determination of haemoglobin concentration. A standardized
questionnaire will be administered to the parents/guardians of the study subject, to collect
information regarding illness that had occurred since the last visit, symptoms experienced,
use of healthcare facilities and use of medicines. Information on the use of bed nets will
be collected again at this visit.
3.10. Assessment of adverse events To determine the prevalence of minor side effects
following drug administration such as headache, fever, weakness, abdominal pain, anorexia,
nausea, vomiting, diarrhoea, rash, itching or sleep disorder participants in each treatment
group are to be visited at home three and seven days after each round of drug administration
and a side effects questionnaire completed. Field workers who complete these questionnaires
will be unaware of the treatment group to which the child belongs. To help establish whether
these adverse events are drug related, the same questionnaire will be administered once
after each treatment round, to 286 children who are not part of the trial, recruited from
nearby villages and matched for age to children in the trial.
Any serious adverse event that occurs during the study period will be reported to the Local
Safety Monitor and Chairman of DSMB.
Primary end-point:
- Incidence of any adverse events during the observation period.
Secondary endpoints:
- Mean Hb (g/dl) at the end of malaria transmission.
- Prevalence of malaria parasitaemia at the end of the malaria transmission season.
- Number of OPD attendances with malaria that meet the case definitions as indicated
below during the surveillance period.
Data management and analysis All baseline, surveillance and laboratory data will be
collected on forms designed for the trial. Field and laboratory staff will be trained to
follow the procedures set out in a series of Standard Operating Procedures (SOPs). Key data
will be double entered and inconsistencies checked; range checks will be used for standard
variables. Primary analyses will be performed on an intention to treat (ITT) basis. Any
child who receives a first dose of drug will be included in the ITT analysis. Children who
are randomised but who do not receive any mediation will not be included in this analysis.
Sample size calculations Drugs for IPT need to be acceptable and have low frequency of
adverse events. If the frequency of adverse events is 20% in the SP/AQ group, a trial with
286 children per arm has 90% power to detect a halving in the frequency of adverse events,
using a significance level of 0.05, or a reduction to 9% or less if a significance of 0.025
is used (to preserve an overall type 1 error rate of 5% for the primary endpoint when there
are 2 comparisons, each alternative drug group with SP/AQ). If the frequency of adverse
events is 15%, a reduction to 5% or less can be detected with the same power, and if the
frequency is 10% a reduction to 2% or less can be detected. Based on experience from several
studies the drop-out rate is not expected to exceed 15% and is likely to be less. Allowing
for 15% drop out, a sample size of 286*3/(1-0.15)=1009 is needed.
Withdrawal during the study:
Study subjects may be withdrawn from the study for any one of the following reasons.
1. Withdrawal of parental / legal guardian's consent.
2. Serious adverse event attributable to the study drug.
3. Loss to follow-up.
Children who develop adverse events attributable to study drugs should not receive further
doses but should be followed-up to monitor safety until the resolution of the adverse
reaction.
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