Malaria Clinical Trial
Official title:
A Randomized Trial of Azithromycin + Artesunate v Artemether-lumefantrine in Uncomplicated Malaria in Tanzanian Children.
This trial sets out to determine whether the combination of azithromycin and artesunate
(AZ+AS) is as good as the current standard treatment for uncomplicated malaria in Tanzania,
artemether-lumefantrine (AL). There are two reasons this is important
1. there are only a limited range of drug combinations which work against malaria in this
area of Tanzania
2. azithromycin has antimalarial properties, but is also a broad-spectrum antibiotic, so
if the combination is an effective antimalarial it might have a place where there are
no diagnostic facilities as syndromic treatment for fever.
Artesunate and azithromycin have both been used alone or in combination with other drugs in
children in Tanzania for many years, and are considered safe. There is trial evidence for
the effectiveness of this combination in adults in Asia, as well as in-vitro (laboratory)
evidence that it works against the malaria parasite.
The trial randomizes children with non-severe malaria to the new combination AZ+AS or the
standard care arm AL. The primary outcome is the parasitological failure rate by day 28-
meaning do malaria parasites get cleared, and stay cleared for at least 28 days. Secondary
outcomes include safety.
Trial drugs. Artemether-lumefantrine (AL) has been selected to be the drug used to treat
uncomplicated malaria in Tanzania. There is extensive efficacy, effectiveness and safety
data on this combination from Tanzania. Artesunate is a key component of most ACTs. It
should not be used as monotherapy, but is highly effective as an antimalarial when used in
combination with another drug with antimalarial properties. There are now many years of
experience of artesunate combinations on Africa and it appears safe in children.
Azithromycin is licensed for use in childhood infections and trachoma. It is well tolerated
and appears very safe in children; for example it does not have the effects of occasional
bone-marrow toxicity seen with chroramphenicol, or the skin reactions sometimes seen with
sulpha-drugs. It is active against the majority of childhood bacterial infections. There is
extensive safety data on azithromycin, including data on azithromycin safety and
tolerability in African children. Azithromycin has been shown to have significant
antimalarial activity in vitro. There is good in vitro data on artemisinin + azithromycin
combinations against malaria including tests for interactions . As a prophylactic drug
against malaria azithromycin is effective in both West and East Africa.
Azithromycin-artesunate has been used as an antimalarial drug combination in Asia. There is
experience from small trials of combinations of artemisinin drugs and azithromycin to treat
P. falciparum in Southeast Asia which were less effective than artesunate-mefloquine and
artemether-doxycycline but several factors, especially the low doses of azithromycin used in
two of these studies and patterns of antibiotic use locally may well have contributed to
this; the combination appears safe . This contrasts with the evidence in East Africa that
azithromycin is an effective antimalarial when used for prophylaxis, and there are several
reasons why it may well be more effective in East Africa than in SE Asia.
Objectives. The overall study objectives will therefore be to compare the efficacy of
azithromycin-artesunate and artemether-lumefantrine in the treatment of non-severe
falciparum malaria in children in an area of high antimalarial drug resistance.
Specific objectives are i) to compare the effects of the drugs on parasitological failure
rates at 28 days in each arm, both unadjusted and adjusting for reinfection judged by
genotyping ii) to compare the drugs for clinical failure rate at 28 days. iii) to compare
the drugs for clinical and parasitological failure at day 42. iv) to compare the drug
combinations for adverse events and side effects v) to undertake a cost-effectiveness
analysis of the two drug combinations.
Study design.
A randomised controlled trial of azithromycin-artesunate and artemether-lumefantrine for the
treatment of non-severe falciparum malaria in children between 6 months and 5 years old.
The trial will be conducted among children attending the MCH clinic in one of the hospitals
in the Tanga region (Muheza Designated District Hospital) with symptoms compatible with
malaria. Those with malaria parasites in their blood smear will be considered for inclusion.
The trial
1. A randomised, open-label trial will be carried out. The slide reader assessing the
primary endpoint will be blind to treatment allocation, and analysis performed by
intention-to-treat.
2. All study drug regimens will be oral. After educating the patient on the need to
complete the course prescribed by the clinician, drugs will be administered as direct
observed therapy (DOT) by a nurse of the study team for morning doses and the evening
dose (AL only) will be taken at home.
Screening.
Patients with non-severe (WHO definition) slide proven malaria with >2000 parasites/microL
will be recruited from the Maternal and Child Health (MCH) clinic of Teule Hospital
following initial pilot studies to identify and solve logistic or other problems.
Project nurses will interview parents/guardians of all febrile children and of those with a
recent (past 48 hours) history of fever to exclude other causes of fever. Those who are
clearly seriously unwell (unconscious, fitting etc) will be triaged immediately to the
emergency admissions team. Those with a fever or history of fever will be referred for rapid
diagnostic testing (RDT) with blood taken by fingerprick. A slide will be taken at the same
time, to be used by the study team or hospital team if appropriate. If RDTs are positive a
study slide will be made, stained and read and they will be referred to the study physician;
if RDTs are negative to the Teule hospital doctor. Duplicate thick and thin blood smears
will be made from all probable malaria cases, Giemsa stained at pH 7.2, and examined
microscopically. All patients seen by the study team will be re-assessed by the physician of
the study team to exclude concomitant infection(s).
Regimen allocation
Random number generated by the computer will be allocated to the two study regimens in
blocks of random size. Patients consenting to participate in the study will be registered
numerically as they present. The registration (enrolment) number of each patient will
determine the drug regimen to be given. Registration numbers will correspond to sealed
opaque envelopes with treatment allocation. Opening an envelope will be deemed to be
randomisation, and intention to treat analysis will proceed on that basis
Once randomised, the child will be treated with the study drug they are allocated unless
they withdraw or are withdrawn from the study.
Follow-up
Patients would be observed on days 0,1,2,7,14,28 and 42. Finger-prick for malaria blood
slide, haemacue and filter paper blood specimen for genotyping will be taken on days 0, 2,
7, 14, 28 and 42 or any day the child presents unwell, and venous blood drawn for a full
blood count and liver enzymes on days 0 and 14.
Rescue medication
Quinine at a dose of 10-mg/kg body weight for 7 days will be the rescue medication, as per
Tanzanian national guidelines.
1. If patients are found to have deteriorating clinical condition in the presence of
asexual parasites from days 0-3 of treatment this will be deemed an early treatment
failure; they will be admitted for parenteral treatment.
2. If patients develop severe or complicated malaria (WHO) at any other stage they will be
admitted for parenteral treatment.
3. Patients who recrudesce with or without symptoms during the study period will be
treated with oral quinine and visited every day by VHCs to support the guardian and
detect any problems early. If there is any sign of deterioration or unexpected side
effects they will be admitted. At day 7 post commencing rescue treatment all patients
will have a blood film; if this is positive they will be admitted for directly observed
therapy.
4. Patients who recrudesce after quinine treatment will be treated as inpatients according
to local guidelines.
Recrudescence versus reinfection.
Blood for PCR will be collected from all patients at enrolment and on follow-up as outlined
above. PCR analysis of parasite genes will be performed only in patients with re-appearance
of parasitaemia in order to differentiate between re-infection and recrudescence.
Adverse events If a patient is unable to tolerate the trial medication the reason for
discontinuation will be recorded in the Clinical Record Form as an "adverse event" and
alternative rescue medication initiated.
Any significant clinical or laboratory abnormality as judged by the senior attending
physician (PI) will be recorded as an adverse event.
Assessment of efficacy; primary outcome: day 28 slide clearance
The day of first treatment is day 0. The day 28 slide clearance rate is the primary end
point of therapeutic efficacy for this trial. It is the proportion of treated patients with
no asexual parasitaemia double-read by microscopists blind to treatment allocation, and who
did not receive rescue medication within that period.
Assessment of efficacy; secondary endpoints. All analysis intention-to treat unless
otherwise specified.
i) Day 14 slide clearance rate by slides double-read blind to treatment allocation ii)
Clinical failure rate on or by day 28 iii) Clinical failure rate on or by day 14 iv)
Parasitological and clinical failure at day 42 v) Day 28 recrudescence rate assessed by PCR
vi) Day 14 and 42 recrudescence rate assessed by PCR vii) Day 28 hemoglobin level viii)
Differences in side effects/AE between groups ix) A per-protocol analysis for all day 14 and
day 28 outcomes
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Single Blind (Outcomes Assessor), Primary Purpose: Treatment
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