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Clinical Trial Details — Status: Active, not recruiting

Administrative data

NCT number NCT05567016
Other study ID # DMID protocol 21-0046
Secondary ID U01AI155315
Status Active, not recruiting
Phase N/A
First received
Last updated
Start date July 18, 2023
Est. completion date November 28, 2025

Study information

Verified date January 2024
Source University of California, San Francisco
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This trial will assess the long-term health and socioeconomic impact of interventions targeting low-density malaria infection (LMI) among children in Tanzania


Description:

This is a 3-arm open-label randomized control trial of 600 children aged 6 months to 10 years in Tanzania, where transmission is low and a high proportion of infections are low-density. Standard of care based on passive case detection (PCD) using rapid diagnostic test (control arm) will be compared to two different approaches to detect and treat P. falciparum LMI: active case detection using molecular testing (ACDm) and PCD using molecular testing (PCDm). Aims are: 1. To assess the impact of standard PCD plus ACDm vs standard PCD on long-term child health 2. To assess the impact of PCDm vs standard PCD on long-term child health 3. To evaluate the cost-effectiveness of ACDm and PCDm


Recruitment information / eligibility

Status Active, not recruiting
Enrollment 600
Est. completion date November 28, 2025
Est. primary completion date November 28, 2025
Accepts healthy volunteers Accepts Healthy Volunteers
Gender All
Age group 6 Months to 10 Years
Eligibility Inclusion Criteria: 1. 6 months to 10 years of age of age at enrollment 2. Primary residence in the study area during the study period 3. Agree to come to study clinic for any illness 4. Agree to avoid medications outside the study, even herbal medication Exclusion Criteria: 1. Another child from household already randomly selected for recruitment 2. Not able or does not provide informed consent 3. Need for emergency intervention 4. Known history of chronic illness requiring regular specialty care including diabetes mellitus, cancer, or Stage 3 or 4 HIV/AIDS 5. Contraindications to artemether-lumefantrine (AL) including history of allergic reaction, weight under 5 kg 6. Participation in another active/ongoing intervention trial

Study Design


Related Conditions & MeSH terms


Intervention

Other:
Active case detection using molecular testing (ACDm)
In the ACDm arm, children will receive ACD using RDT and qPCR 3x yearly with treatment using artemether-lumefantrine (AL) if RDT or qPCR positive. With fevers, participants will receive standard PCD using RDT.
Passive case detection using molecular testing (PCDm)
With fevers, participants will receive PCDm, in which qPCR will be done in RDT negatives with treatment using AL if positive.
Control (standard of care)
With fevers, participants will receive standard PCD using RDT with treatment using AL if positive.

Locations

Country Name City State
Tanzania Kiwangwa and Fukayosi clinics Bagamoyo

Sponsors (6)

Lead Sponsor Collaborator
University of California, San Francisco Chan Zuckerberg Biohub, Ifakara Health Institute, National Institute of Allergy and Infectious Diseases (NIAID), Stanford University, Swiss Tropical & Public Health Institute

Country where clinical trial is conducted

Tanzania, 

Outcome

Type Measure Description Time frame Safety issue
Primary Incidence of all-cause sick visits Number of sick visits to health facility per person time, excluding planned admissions for medical care, elective surgery, and trauma. 24 months from enrollment
Secondary Prevalence of anemia Proportion of routine Hb measurements that are low (<11 g/dL) or moderate-severe low (<8 g/dL) 24 months from enrollment
Secondary Prevalence of underweight status Prevalence of underweight status will be defined as the percentage of participants with low weight for age z-scores of less than -2. The World Health Organization (WHO) anthropometric indices will be utilized for standards. 24 months from enrollment
Secondary Prevalence of stunting Prevalence of stunting will be defined as the percentage of participants with low height for age z-scores of less than -2. The World Health Organization (WHO) anthropometric indices will be utilized for standards. 24 months from enrollment
Secondary Prevalence of wasting Prevalence of wasting will be defined as the percentage of participants with low weight for height z-scores of less than -2. The World Health Organization (WHO) anthropometric indices will be utilized for standards. 24 months from enrollment
Secondary Prevalence of malnutrition Prevalence of malnutrition will be defined as the percentage of participants with a z-score of -3 to -2 indicating moderate malnutrition or a z-score of less than -3 indicating severe malnutrition in any of the following: weight for age, height for age, or weight for height. 24 months from enrollment
Secondary Prevalence of vomiting following administration of study drugs Vomiting immediately or within 30minutes following administration of study drugs and measures of non-adherence. 24 months from enrollment
Secondary All-cause fever episodes Number of documented fever episodes (axillary temperature of =37.5°C) per person time and number of fever episodes (documented and reported) per person time 24 months from enrollment
Secondary Incidence of clinical symptoms Number of days with overall symptoms reported as moderate (=3 on a 5-point scale) per person time 24 months from enrollment
Secondary Incidence of clinical malaria New episodes of positive malaria test (with fever or other clinical symptoms) per person time 24 months from enrollment
Secondary Proportion of fever episodes with clinical failure Proportion of fever episodes that lead to clinical failure, defined as persistent or worsening symptoms assessed 7 and 28 days after initial evaluation. 24 months from enrollment
Secondary Prevalence of parasitemia Proportion of routine samples with parasites detected by microscopy or quantitative polymerase chain reaction (qPCR). 24 months from enrollment
Secondary Incidence in antibiotics prescribed Number of antibiotic regimens prescribed per person time 24 months from enrollment
Secondary Cognitive ability among children 0-3.4 years of age on the Global Scales of Early Development (GSED) GSED is a validated instrument that measures population-level early childhood development. The tool measures children's early skills and behaviors in four primary domains: motor, cognitive, language, and social-emotional development.Measures will be normalized within our sample to mean 0 and standard deviation 1, with higher scores indicating better test performance. 24 months from enrollment
Secondary Cognitive ability among children 3.5-5 years of age on the International Development and Early Learning Assessment (IDELA) The IDELA is a validated, global tool that uses direct child assessment to measure early learning and development across 4 core domains (Emergent Literacy, Emergent Numeracy, Motor, Social-emotional). Scores range from 0-100% as a percentage of correct tasks averaged across the 4 domains. Measures will be normalized within our sample to mean 0 and standard deviation 1, with higher scores indicating better test performance. 24 months from enrollment
Secondary Cognitive ability among children 6-12 years of age on the East Africa Neurodevelopment Assessment Tool The East African Neurodevelopment Assessment Tool is a locally adapted modification of the Kaufman Brief Intelligence Test 2nd Ed. The test assesses 3 core metrics including general intelligence, executive function, literacy skills - in addition to behavioral and emotional development. Measures will be normalized within our sample to mean 0 and standard deviation 1, with higher scores indicating better test performance. 24 months from enrollment
Secondary Sustained attention among children 5-8 years of age on the Pencil Tapping Test The pencil tapping test is one of the tasks in the Preschool Self-Regulation Assessment (PSRA) and is used to assess inhibitory control in younger children. The child and an assessor have pencils, and child is instructed to tap one/two times(s) depending on what assessor does, with the number of correct responses scored. Measures will be normalized within our sample to mean 0 and standard deviation 1, with higher scores indicating better test performance. 24 months from enrollment
Secondary Sustained attention among children 9-12 years of age on the Code Transmission Test, a local adaptation of the Test of Everyday Attention for Children(TEA-Ch) Code transmission test is a sub-test of Test of Everyday Attention for Children (TEA-Ch) used for assessment of sustained attention in children. In the test, the child must remember spoken digits, and remember the digit that comes before sequence of numbers. Child is scored on completed and correct answers. Measures will be normalized within our sample to mean 0 and standard deviation 1, with higher scores indicating better test performance. 24 months from enrollment
Secondary Incidence of school absenteeism The number of days of school absenteeism for any reason including illness. 24 months from enrollment
Secondary School performance School performance will be defined as the incidence of school advancement to the next grade. 24 months from enrollment
Secondary Socioeconomic costs to participant Estimated long-term income loss due to impaired early childhood development 24 months from enrollment
Secondary Socioeconomic costs to family Total caregiver-reported costs of sick visits and transport to sick visits plus estimated loss of income from number of days of caregiver work absenteeism. 24 months from enrollment
Secondary Socioeconomic costs to health system Estimated costs of testing and treatment for caregiver-reported number of sick visits. 24 months from enrollment
Secondary Cost effectiveness Cost per outcome averted (e.g., per sick visit averted, per disability adjusted life years (DALYs), and per economic dollar saved, etc.) 24 months from enrollment
Secondary Prevalence of systemic inflammation Proportion of sick visits with elevated elevated C-reactive pep-tide (CRP) 24 months from enrollment
Secondary Proportion with antimalarial antibodies against P.falciparum Percentage of patients with antimalarial antibodies 24 months from enrollment
Secondary Proportion with biomarkers of inflammation Percentage of patients with elevated cytokines 24 months from enrollment
Secondary Proportion with general antibody responses to vaccines Percentage of patients with vaccine antibodies 24 months from enrollment
Secondary Proportion with general antibody responses to common pathogens Percentage of patients with common pathogen antibodies 24 months from enrollment
Secondary Incidence of adverse events (AEs) Number of AEs per person time. AEs will be considered as any grade 3-4 AE or serious adverse event (SAE); individual AEs; or AEs related to study drugs. 24 months from enrollment
Secondary Incidence of wasting Incidence proportion of wasting will be defined for each age range of measurement. It is defined as the proportion of children not wasted at the start of the period who became wasted during the age period (the proportion of children who had the onset of new episodes during the period). Incident wasting episodes are defined as a change in weight-for-length z-scores from above -2 Z in the prior measurement to below -2 Z in the current measurement. We will define incident severe wasting analogously using a -3 Z cutoff. We will assume a 60-day washout period before a new wasting episode could occur. 24 months from enrollment
Secondary Incidence of stunting Incidence proportion of stunting will be defined for each age range of measurement. It is defined as the proportion of children not stunted at the start of the period who became stunted during the age period. Incident stunting episodes will be defined as a change in length-for-age z-scores from above -2 Z in the prior measurement to below -2 Z in the current measurement. We will define incident severe stunting analogously using a -3 Z cutoff. 24 months from enrollment
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