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| Name | Class |
|---|---|
| Mahidol Oxford Tropical Medicine Research Unit | OTHER |
| Kinshasa Medical Oxford Research Unit | UNKNOWN |
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A randomised open labeled, parallel-group, controlled trial to assess the efficacy of paracetamol to reduce kidney dysfunction caused by cell-free haemoglobin-mediated oxidative damage in paediatric patients with falciparum malaria complicated by intravascular haemolysis.
Kidney dysfunction is an independent predictor of mortality in both adults and children with severe malaria. In the largest studies of paediatric severe malaria, approximately 25% of children had kidney dysfunction and these patients accounted for roughly 50% of total deaths.
Although the multifactorial mechanism of severe malaria-associated AKI has primarily been studied in adults, evidence suggests that similar mechanisms of renal injury are involved in paediatric severe malaria. Cell-free haemoglobin (CFH) -mediated oxidative damage has recently been recognized as an important pathway in a range of common conditions, including rhabdomyolysis, primary pulmonary graft dysfunction, and haemolytic disorders, such as post-cardiac surgery, and malaria. During malaria infection, there is haemolysis of parasitized and uninfected red blood cells (RBCs). CFH-mediated lipid peroxidation generates F2-isoprostanes (F2-IsoPs) and isofurans (IsoFs), which are considered robust in vivo measures of oxidative stress. F2-IsoPs are potent renal vasoconstrictors that act via thromboxane A2 receptors. Both F2-IsoPs and IsoFs have been associated with AKI in patients with rhabdomyolysis, sepsis, adults with severe malaria and haemolysis post-cardiopulmonary bypass (CPB). Further, elevated haemin and CFH concentrations were associated with mortality. In a cohort of children with severe malaria, elevated haem-to-haemopexin ratio was associated with stage 3 AKI, and 6-month mortality. These studies demonstrate that intravascular haemolysis occurs with increasing severity in paediatric malaria. Haem redox cycling between ferric (Fe3+) and ferryl (Fe4+) states generates globin radicals, inducing lipid peroxidation. These data suggested that haemolysis induces oxidative damage, and CFH-mediated oxidative damage contributes to AKI complicating paediatric malaria.
A novel mechanism of paracetamol was recently demonstrated, showing that paracetamol acts as a potent inhibitor of haemoprotein-catalyzed lipid peroxidation, by reducing ferryl haem to its less toxic ferric state and quenching globin radicals. We hypothesize that this novel inhibitory mechanism of paracetamol may provide renal protection in children with severe malaria by reducing the haemoprotein-induced lipid peroxidation. As there is currently no consensus that exists concerning adequate medical treatment for severe malaria complicated by intravascular haemolysis and AKI, the potential application of this safe and extensively used drug would be of great benefit.
The study will be a randomised, open-labelled, controlled trial. Randomisation will be stratified into two groups : (i) Patients with no acute kidney injury (AKI) at enrolment, and (ii) Patients with AKI at enrolment. Both groups will be randomised into two arms: Arm 1: Paracetamol 15 mg/kg/dose 6 hourly for 72 hours Arm 2: Mechanical antipyresis if fever in the first 72 hours. All patients will receive intravenous artesunate followed by artemether-lumefantrine as soon as they are able to take oral medication or according to medical judgment.
The study will be conducted at the Kinshasa Medical Oxford Research Unit (KIMORU, Democratic Republic of the Congo, DRC). The recruitment phase of the study is expected to last 18 months, from September 2021 - February 2022. The total time to complete the study will be approximately 3 years.
Funder: Canadian Institutes of Health Research
CIHR grant reference number : PJT-162116
UBC grant number: 20R01487
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Arm 1 | Experimental | Paracetamol 15 mg/kg/dose 6 hourly for 72 hours |
|
| Arm 2 | Sham Comparator | Mechanical antipyresis (i.e. loose clothing, tepid sponging, fanning and cooling blanket) if fever in the first 72 hours. |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Paracetamol | Drug | Paracetamol 15 mg/kg/dose IV 6 hourly for 72 hours |
|
| Measure | Description | Time Frame |
|---|---|---|
| Acute kidney injury (AKI) or death among patients enrolled without AKI (Composite outcome) | Composite outcome of development of AKI (defined as creatinine ≥26.5 µmol/L or ≥1.5x baseline), or death at any timepoint | during first 7 days of enrolment |
| Acute kidney injury (AKI) progression or death among patients enrolled with AKI (Composite outcome) | Composite outcome of worsening of AKI (defined as creatinine ≥2x baseline, or ≥3x baseline, or initiation of RRT or eGFR <35 ml/min/ 1.73 m2) or death at any timepoint. | during first 7 days of enrolment |
| Measure | Description | Time Frame |
|---|---|---|
| Number of patients with serious adverse events | Number of patients with serious adverse events (mortality and/or hepatotoxicity, as defined by Hy's Law). | AST/ALT/total bilirubin during the first 5 days from enrolment; mortality assessed Day 0 to 7. |
| Proportion of patients who develop Major Adverse Kidney Events (MAKE) composite |
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Inclusion Criteria:
Male or Female, patients aged 1 to ≤ 14 years
Severe P. falciparum malaria, confirmed by positive blood smear with asexual forms of P. falciparum or positive PfHRP2 rapid diagnostic test (RDT).
Pre-specified modified criteria for severe falciparum malaria
Upon hospital admission, asexual parasitaemia plus at least ONE of the following:
Temperature >38°C on admission or fever during the preceding 48 hours.
Less than 24 hours of antimalarial therapy
Attending caregiver of participant willing and able to give informed consent for participation in the study
Exclusion Criteria:
The participant may not enter the trial if ANY of the following apply:
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| Name | Role | Phone | Extension | |
|---|---|---|---|---|
| Katherine Plewes, Dr. | Contact | +1-604-603-4033 | katherine@tropmedres.ac | |
| Arjen Dondorp, Prof. | Contact | +662-203-6333 | 6303 | arjen@tropmedres.ac |
| Name | Affiliation | Role |
|---|---|---|
| Katherine Plewes, Dr. | Mahidol Oxford Tropical Medicine Research Unit | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| The Kinshasa Medical Oxford Research Unit (KIMORU) | Recruiting | Kinshasa | Congo | Democratic Republic of the Congo |
Participant data and results from blood analyses stored in the database may be shared according to the terms defined in the MORU data sharing policy with other researchers to use in the future. Datasets will be de-identified to ensure patient privacy and confidentiality.
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After completion of trial activities and reporting
MORU Data Sharing Policy. (http://www.tropmedres.ac/data-sharing-policy)
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| ID | Term |
|---|---|
| D008288 | Malaria |
| D016778 | Malaria, Falciparum |
| D058186 | Acute Kidney Injury |
| ID | Term |
|---|---|
| D011528 | Protozoan Infections |
| D010272 | Parasitic Diseases |
| D007239 | Infections |
| D000096724 | Mosquito-Borne Diseases |
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| ID | Term |
|---|---|
| D000082 | Acetaminophen |
| ID | Term |
|---|---|
| D000083 | Acetanilides |
| D000813 | Anilides |
| D000577 | Amides |
| D009930 | Organic Chemicals |
| D000814 |
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Prior to randomization, participants will be stratified into two groups: (i) Patients with no acute kidney injury (AKI) at enrolment, and (ii) Patients with AKI at enrolment. Both groups will be randomised into two arms:
Arm 1: Paracetamol 15 mg/kg/dose 6 hourly for 72 hours
Arm 2: Mechanical antipyresis
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| Mechanical antipyresis | Procedure | Mechanical antipyresis (i.e. loose clothing, tepid sponging, fanning and cooling blanket) if fever in the first 72 hours. If a temperature >38.5°C persists despite mechanical antipyresis, or if deemed necessary by the treating clinician, then paracetamol can be administered according to local practice (paracetamol IV 15 mg/kg as needed). |
|
Major Adverse Kidney Events (MAKE) composite, defined as ≥ 1 efficacy renal endpoints: (i) death, (ii) need for renal replacement therapy, (iii)≥ 50% reduction in eGFR from baseline to 90 days. |
| 90 days |
| Fever clearance time | Time taken for aural temperature: (i) to fall < 37.5°C (FCT-A), and (ii) to fall < 37.5°C and remain there for >24 h (FCT-B) | 6-hourly temperature assessments during first 7 days from enrolment |
| Coma recovery | Time until Glasgow Coma Score (GCS) return to 15 (or Blantyre Coma Score (BCS) return to 5 in preverbal children) | 6-hourly GCS/BCS assessments during first 7 days from enrolment |
| Longitudinal change in renal function | As measured by creatinine concentration (umol/L) | During the first 7 days from enrolment |
| Longitudinal change in markers of hemolysis | As measured by cell-free haemoglobin (ug/mL), haemopexin (ug/mL), haptoglobin (ug/mL), haem (uM), F2-isoprostane (pg/mL) and isofurans (pg/mL) concentrations | during the first 3 days from enrolment |
| Longitudinal change of endothelial activation | As measured by concentrations of angiopoietin-Tie2 pathway markers (i.e. Ang-1, Ang-2, sTie2, sTie1) | during the first 3 days from enrolment |
| Longitudinal change of immune activation | As measured by soluble triggering receptor expressed on myeloid cells concentration (sTREM-1; pg/mL) | during the first 3 days from enrolment |
| Longitudinal change of AKI biomarker | As measured by cystatin-C concentration (Cys-C; ug/mL) | during the first 3 days from enrolment |
| Parasite (parasites/ul) clearance | as measured by time until two consecutive negative smears (hours), and by rate using the parasite clearance estimator to determine slope half-life (hours) from 12-hourly parasite counts. | 12-hourly parasitemia assessments during first 7 days from enrolment |
| Exploratory analysis with sex | Primary efficacy analyses will be analysed using a logistic regression model to obtain odds ratios, comparing the odds of a combined endpoint of kidney function deterioration or death between treatment groups. A multivariable model including an interaction term (sex and treatment) will be assessed in the primary analyses to explore potential differences between males and females. | During first 7 days from enrolment |
| Pharmacokinetic properties | Population pharmacokinetic model (relative bioavailability, mean transit absorption time (hours), apparent oral elimination clearance (L/hours), apparent volume of distribution (L) | during the first 24 hours from enrolment |
| Pharmacokinetic properties | Peak plasma concentration (Cmax; mg/L) | during the first 24 hours from enrolment |
| Pharmacokinetic properties | Time to peak plasma concentration (Tmax; hours) | during the first 24 hours from enrolment |
| Pharmacokinetic properties | Terminal elimination (t1/2; hours) | during the first 24 hours from enrolment |
| Pharmacokinetic properties | Area under the plasma drug concentration-time curve (AUC0-24; mg×h×L-1) | during the first 24 hours from enrolment |
| Pharmacodynamic relationships | Pharmacodynamic effects on creatinine concentration (mol/L) | during first 7 days from enrolment |
| Pharmacodynamic relationships | Pharmacodynamic effects on liver toxicity, as measured by AST and ALT (U/L) | during first 7 days from enrolment |
| Pharmacodynamic relationships | Pharmacodynamic effects on temperature (Celsius) | during first 7 days from enrolment |
| Pharmacodynamic relationships | Pharmacodynamic effects on parasitemia, as measured by parasites/ul and slope half-life | during first 7 days from enrolment |
| Pharmacodynamic relationships | Pharmacodynamic effects on GCS (or BCS in pre-verbal children) | during first 7 days from enrolment |
| D000079426 |
| Vector Borne Diseases |
| D051437 | Renal Insufficiency |
| D007674 | Kidney Diseases |
| D014570 | Urologic Diseases |
| D052776 | Female Urogenital Diseases |
| D005261 | Female Urogenital Diseases and Pregnancy Complications |
| D000091642 | Urogenital Diseases |
| D052801 | Male Urogenital Diseases |
| Aniline Compounds |
| D000588 | Amines |