Malaria Clinical Trial
Official title:
A Randomized Clinical Trial to Measure the Impact of Retreatment With an Artemisinin-based Combination on Malaria Incidence and Its Potential Selection of Resistant Strains
This is a bi-centric phase IIIb, randomized, open label, 3-arm clinical trial performed to
investigate the impact of retreatment with an Artemisinin-Based Combination (ACT), for
example Arthemeter-Lumefantrine (AL) in Uganda (Ug) and artesunate-amodiaquine (ASAQ) in
RDCongo, on malaria incidence and its potential selection of resistant strains.
Patients will be followed-up for efficacy and safety during 42 days after treatment with the
first line therapy recommended by the national authorities(arthemeter-lumefantrine in Uganda
and artesunate-amodiaquine in RDCongo) and retreated the patients either with the same ACT
or an other ACT or oral Quinine + clyndamicin.
The investigators hypothesize that (re)treatment with the first line ACT treatment beyond 14
days is as efficacious as any other rescue treatment, without the risk of selecting drug
resistant strains.
RATIONALE Following the World Health Organization (WHO) guidelines, most African countries
have opted for ACT. Several clinical trials on ASAQ, an ACT, completed in Africa have shown
an efficacy > 90% (3-5). Furthermore, after The polymerase chain reaction (PCR) analysis,
over 75 % of ASAQ & AL treatment failures have been classified as new infections, while
recrudescences have low parasite densities. ASAQ is safe and easy administered, with a good
treatment adherence. Therefore, effectiveness may be close to efficacy . ASAQ has now been
developed as fixed-dose combination and registered. The Democratic Republic of Congo (DRC)
has also chosen ASAQ as first-line treatment for uncomplicated malaria.
Efficacy of the 6 dose regimen of AL has been demonstrated in semi-immune and non-immune
populations in Asia and Africa to be consistently greater than 95%, with rapid parasite and
symptom clearance and significant gametocidal effect. In Uganda, AL has already been chosen
as first-line treatment for uncomplicated malaria.
In DRC and Uganda, quinine is the rescue treatment for malaria. It is cheap, widely
available and generally considered to be effective but is not popular due to the unwanted
side effects. Quinine has a very short half life, therefore repeated dosing is required. In
an efficacy study of quinine and artemisinin for uncomplicated malaria in Vietnam,
recrudescence rates were 16% after 7 days of quinine monotherapy. In studies conducted in
Gabon, Plasmodium falciparum in Vitro sensitivity to quinine was high and had not changed
over the past decade. Although quinine monotherapy shows high efficacy in the setting of
clinical trials, it has considerable disadvantages, mainly because of its poor tolerability
and the prolonged treatment course. Poor adherence carries a high risk of treatment failure,
particularly because quinine causes a syndrome of adverse effects known as cinchonism that
includes primarily tinnitus, nausea, and vertigo. Other reported side effects are high tone
hearing impairment, dizziness, hypotension as well as headache and visual disturbances. As
result of these side effects, some studies have reported poor compliance to treatment. A
randomized trial in Thailand reported 71% adherence Such poor adherence to the 7-days
regimen is associated with a high risk of treatment failure, which can contribute to the
development and spread of resistance. Furthermore, in field circumstances patients are often
re-treated with the recommended first line drug, i.e. ASAQ.
As quinine is effective against all species of malaria including chloroquine-resistant
strains of P. falciparum, it is widely used for the treatment of severe malaria. Therefore,
it should be protected from resistance by a rational use, as its effectiveness in
uncomplicated malaria is lower than ACT.
Rationale Considering the facts that: over 90% of treatment failure to ASAQ or AL are new
infections, parasitaemia is low in case of recrudescence occurring from day 14 and in
real-life situations patients are re-treated with the same first line drug, there is the
need to assess the role of the first line treatment as rescue treatments. This efficacy will
be compared to quinine + clindamycin and another ACT treatment in line with the WHO
guideline, and another ACT treatment to provide clear guidelines. The investigators
hypothesize that re-treatment with the first line ACT treatment beyond 14 days is as
efficacious as any other rescue treatment, without the risk of selecting drug resistant
strains. Furthermore, a prolonged follow up will allow the assessment of the
epidemiological, parasite related risk factors for repeated malaria infection and to collect
samples for immunological risk factors for repeated malaria attacks.
TRIAL OBJECTIVES AND PURPOSE
Efficacy
The primary objective is:
1. to show that, in children aged 12 to 59 months with recurrent uncomplicated P.
falciparum malaria within 42 days of treatment with an artemisinin-based combination
therapy (ASAQ in DRC or AL in Uganda), the PCR adjusted efficacy at 28 days after
re-treatment with the same artemisinin-based combination therapy is at least 90% and
2. to estimate the relative efficacy of re-treatment with the same artemisinin-based
combination compared to treatment with quinine and treatment with another
artemisinin-based combination therapy (ASAQ after first line AL treatment or AL after
first line ASAQ treatment).
Secondary objectives are:
1. To evaluate the PCR-unadjusted efficacy at 28 days of re-treatment with the same
artemisinin-based combination therapy and to compare it to treatment with quinine +
clindamycin and treatment with another artemisinin-based combination therapy (ASAQ
after first line AL treatment or AL after first line ASAQ treatment).
2. To evaluate and compare the efficacy of AL, ASAQ and quinine + clindamycin as rescue
treatment for a recurrent P. falciparum malaria episode occurring 2 weeks after the
administration of the first line treatment, with and without PCR adjustment.
3. To evaluate and compare the 42 days clinical efficacy of AL (Uganda) and ASAQ (RDC) for
the first line treatment of uncomplicated P. falciparum malaria, with and without PCR
adjustment.
4. To evaluate and compare the efficacy of the different rescue treatment regimens in
terms of fever clearance time, asexual parasite clearance time, gametocytaemia at day
7, 14, 21 and 28, and, Hemoglobin changes between day 0 and days 14 and 28.
Additional objectives are:
1. To evaluate the selection of Plasmodium falciparum pfmdr1 alleles following therapy
with quinine + clindamycin, AL and ASAQ.
2. To assess epidemiological, parasitological and host related predictors for recurrent
malaria infections, an adjacent study that will be developed in a separate nested study
protocol.
Safety To evaluate the safety and tolerability of AL, ASAQ and quinine + clindamycin when
used as rescue treatments.
DRUG TO BE TESTED Quinine Quinamax® (Sanofi) + Clindamycin Dalacin® (Pfizer): in this study
the investigators will use Dalacin syrup (75mg/5ml) and dry Quinamax® tablets (125mg) of
whom the dosage is not adapted to children below 9 kg. The latter explains why children
below 12 months will be exclude from our study
Artemether-lumefantrine (AL) AL of Novartis, marketed under the trademarks Riamet® and
Coartem®, was registered in Switzerland in 1999, it is pre-qualified by the WHO and has
since received marketing authorisation in several endemic and non-endemic countries. A
recent review showed that the drug combination is highly efficacious against sensitive and
multidrug resistant falciparum malaria as it offers the advantage of rapid clearance of
parasites by artemether and the slower elimination of residual parasites by lumefantrine.
Amodiaquine artesunate ASAQ is safe, easy to use and efficacious and the second most used
ACT worldwide. DRC, through the National Malaria Control Program has complied with the WHO
recommendation by recommending since 2005 ASAQ as first line treatment for uncomplicated
malaria. In a study conducted in 2004 in the eastern part of the country, the efficacy of
ASAQ was estimated at 93% after PCR adjustment. Twenty five trials (11,700 patients) carried
out in Sub-Saharan Africa show a PCR-adjusted efficacy at day 28 of 94%. ASAQ is currently
the second most used ACT globally (co formulated Co-arsucam® or ASAQ Winthrop®,
Sanofi-Aventis. A study has been conducted in Burkina Faso in children under 5 and has shown
that co-formulated ASAQ is well tolerated and its efficacy was 93% after PCR correction. The
investigators will use this co-formulated ASAQ Winthrop® of Sanofi-Aventis, age dosed and
put on the market since March 2007. This product has been pre-qualified by the WHO.
STUDY DESIGN This is a bi-centre, phase IIIb, randomized, open label, 3-arm trial.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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