DeTACT-ASIA: A Trial to Compare the Efficacy, Safety and Tolerability of Combinations of 3 Anti-malarial Drugs Against Combinations of 2 Anti-malarial Drugs (Asia)

Study Description

Brief Summary

A partially blinded randomised controlled non-inferiority trial comparing the efficacy, tolerability and safety of Triple ACTs artemether-lumefantrine + amodiaquine (AL+AQ) and artesunate- mefloquine+piperaquine (AS-MQ+PPQ) with the ACTs artemether-lumefantrine + placebo (AL+PBO) and artesunate- mefloquine + placebo (AS-MQ+PBO) (with single-low dose primaquine in some sites) for the treatment of uncomplicated Plasmodium falciparum malaria to assess and compare their efficacy, safety, tolerability.

Detailed Description

Subjects will be randomized to up to four arms: artemether-lumefantrine + amodiaquine, artemether-lumefantrine + placebo, artesunate-mefloquine + piperaquine and artesunate-mefloquine + placebo. As a contingency measure in case of significant differences in the efficacy or safety of one of the combinations being tested and/or study drug expiry or unavailability, subjects may be randomised to 2 arms with a matching ACT-TACT pair, i.e., with artemether-lumefantrine + placebo or artemether-lumefantrine + amodiaquine OR artesunate-mefloquine + placebo or artesunate-mefloquine + piperaquine.

Some sites may randomize between 2 arms only with matching ACT-TACT pairs, i.e., artemether-lumefantrine + placebo or artemether-lumefantrine + amodiaquine OR artesunate-mefloquine + placebo or artesunate-mefloquine + piperaquine.

In the control arms, the ACT will be co-packed with a matched (appearance) placebo.

In lower transmission settings (Annual Parasite Incidence <50 per 1000 population per year) the treatment will include a single 0.25 mg/kg gametocytocidal dose of primaquine as recommended by the WHO for children ≥10 kg. All drug administrations will be observed.

Subjects will be treated in an in-patient unit for 3 days and followed up weekly up to D63. Microscopy to detect and quantify malaria parasitaemia will be performed daily (more frequently in patients with parasite density of >5000/µL at inclusion) during hospitalization, at all weekly and unscheduled visits. A physical examination and measurements of vital signs along with a symptom questionnaire for tolerability will be performed and recorded through a standardized method at baseline, daily during admission and weekly during follow up through D42 and at all unscheduled visits. Physical exam, vital sign measurements and assessments of symptoms will be performed on D49, D56, and D63 only for patients who are parasitaemic or those who report fever or other symptoms. Electrocardiographs will be performed during admission (H0, H4, H52, or H64) and day 42 of follow up to assess and compare the effect of ACTs and TACTs antimalarials on QT or QTc-intervals.

The DeTACT-ASIA Trial is funded by UK Aid from the UK government's Foreign, Commonwealth and Development Office (FCDO). The FCDO project number is 300341-114.

Study Design

Outcome Measures

Primary Outcome Measures

1. Efficacy defined as PCR corrected adequate clinical and parasitological response (ACPR). [42 days]

Secondary Outcome Measures

1. Efficacy defined as PCR corrected adequate clinical and parasitological response (ACPR) [63-day]

2. Efficacy defined as adequate clinical and parasitological response (PCR) [63-day]

3. Efficacy defined as adequate clinical and parasitological response (ACPR) [42-day]

4. Parasite clearance half-life [7 days]

5. proportion of subjects with microscopically detectable P. falciparum parasitaemia [3 days]

6. Fever clearance time [7 days]

   Time taken for the tympanic temperature to fall below 37.5 ºC in patients who were febrile at inclusion

7. Proportion of subjects with gametocytemia during and after treatment stratified by presence of gametocytes at enrolment [63 days]

8. Number of adverse events [42 days]

9. Number of serious adverse events [42 days]

   Including markers of hepatic, renal or bone marrow toxicity

10. Number of cardiotoxicity events [52 or 64 hours depends on treatment arm]

    In particular QTc-interval above 500 ms or an increase > 60 ms above baseline values at timepoint H4 and H52/H64 and between these time points

11. Change in haemoglobin stratified for G6PD status/genotype [28 days]

12. Proportion of subjects requiring retreatment due to vomiting within 1 hour after administration of the study drugs [1 hour]

13. Proportion of subjects that reports completing a full course of observed TACT [3 days]

14. Proportion of subjects that reports completing a full course of observed ACT [3 days]

15. Pharmacokinetic profiles and interactions (including Cmax) of artemisinin-derivatives and partner drugs in ACT and TACT treated subjects in correlation with pharmacodynamics measures of drug efficacy [42 days]

16. Pharmacokinetic profiles and interactions (AUC) of artemisinin-derivatives and partner drugs in ACT and TACT treated subjects in correlation with pharmacodynamics measures of drug efficacy [42 days]

17. Plasma levels of partner drugs in correlation with treatment efficacy and treatment arm [7 days]

Other Outcome Measures

1. Comparison of efficacy, defined as PCR corrected adequate clinical and parasitological response (ACPR) at day 42 versus day 63 [63 days]

2. Comparison of efficacy, defined as adequate clinical and parasitological response (ACPR) at day 42 versus day 63 [63 days]

3. Proportions of recurrent infections with parasites carrying mutations of known functional significance [63 days]

4. Proportions of specimens collected at baseline with parasites carrying mutations of known functional or operational significance [baseline]

   Mutations include pfkelch13, pfcrt, pfmdr1, pfdhfr, pfdhps, pfplasmepsin2 , partial or complete deletions of pfhrp2 and other current parasite genetic markers associated with resistance or identified over the course of the study

5. Number of samples from drug sensitive and resistant parasites that have common genomic patterns that associate with in vivo or in vitro parasite drug sensitivity phenotypes. [63 days]

6. Survival rate or IC50 in in vitro drug susceptibility assay of P. falciparum to artemisinins and partner drugs according to study sites and genotype [63 days]

7. Percent agreement and/or KAPPA score of SNPs assessed from dry blood spots versus from whole genome sequencing in leukocyte depleted blood samples [63 days]

8. Correlation between qPCR based versus microscopy based assessments of parasite clearance dynamics [14 days]

9. Correlation of parasite clearance metrics as assessed by microscopy versus digital microscopy [3 days]

10. Number of samples from drug sensitive and resistant parasites obtained before treatment and 6, 12, and 24 hours after start of treatment that can be assigned to a common transcriptomic pattern. [63 days]

11. Levels of RNA transcription coding for male or female specific gametocytes at admission up to day 14, stratified by the presence of gametocytes at enrolment [14 days]

12. Correlation between the host genotype and the pharmacokinetics and pharmacodynamics of antimalarials [42 days]

    Host genotype (e.g., CYP2D6, CYP3A4, KCNQ1/LQT1, KCNH2/LQT2, SCN5A/LQT3)

13. Correlations between the place of residence, work, recent travel history assessed by interview and mobile phone records to identify behaviours and risk factors associated with malaria infection. [63 days]

14. Correlation between titres of antibodies against malaria parasite antigen and efficacy defined as PCR corrected adequate clinical and parasitological response (ACPR) [63 days]

15. Correlation between titres of antibodies against malaria parasite antigen and efficacy defined as adequate clinical and parasitological response (ACPR) [63 days]

Eligibility Criteria

Criteria

Inclusion Criteria:

• Male or female, >/= 6 months

• Ability to take oral medication

• Acute uncomplicated P. falciparum monoinfection

• Asexual P. falciparum parasitaemia: 96 to 200,000/µL, determined on a peripheral blood film

• Fever defined as >/= 37.5°C tympanic temperature or a history of fever within the last 24 hours

• Written informed consent by the subject or parent/guardian in case of children lower than the age of consent and assent if required (per local regulations)

• Willingness and ability of the subjects or parents/guardians to comply with the study protocol for the duration of the study

Exclusion Criteria:

• Signs of severe malaria (adapted from WHO criteria)

• Patients not fulfilling criteria for severe malaria but with another indication for parenteral antimalarial treatment at the discretion of the treating physician

• Haematocrit < 20% at screening

• Subjects who have received artemisinin or a derivative within the previous 7 days OR lumefantrine or amodiaquine within the previous 14 days OR mefloquine or piperaquine within the previous 30 days

• Acute illness other than malaria requiring systemic treatment

• Severe acute malnutrition

• Known HIV infection

• Known tuberculosis infection

• For females: pregnant, trying to get pregnant or are lactating

• History of allergy or known contraindication to any of the study drugs, including neuropsychiatric disorders and epilepsy

• Previous splenectomy

• Enrolment in DeTACT in the previous 3 months

• Participation in another interventional study in the previous 3 months

Criteria for severe malaria

• Impaired consciousness (Glasgow Coma Scale, Blantyre Coma Scale)

• Prostration

• Respiratory distress (defined as maximal respiratory rate, by age)

• ≥2 convulsions in the past 24 hours

• Circulatory collapse

• Pulmonary edema

• Abnormal bleeding

• Visible jaundice

• Haemoglobinuria (blackwater)

• Hyperparasitaemia (>10%)

Contacts and Locations

Locations

Sponsors and Collaborators

• University of Oxford
• Mahidol Oxford Tropical Medicine Research Unit

Investigators

Study Documents (Full-Text)

More Information

Publications