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Spatial Repellent Products for the Control of Vector Borne Diseases - Malaria - Kenya

Not Applicable
Withdrawn
Conditions
Malaria
Interventions
Device: Spatial Repellent product with active ingredient
Device: Spatial Repellent product without active ingredient (SHIELD)
Device: Active ingredient
Registration Number
NCT02294201
Lead Sponsor
University of Notre Dame
Brief Summary

The primary objective of the study is to demonstrate and quantify the protective efficacy (PE) of spatial repellent products in reducing the incidence of malaria infection in human cohorts. The null hypothesis (H0) is that there is no difference in malaria incidence between intervention and control arms.

Detailed Description

The primary epidemiological endpoint will be the incidence density of first time malaria infections among human cohorts during the follow-up period as detected by polymerase chain reaction assay (PCR). This measure will inform PE (the reduction of incidence) between intervention and control study arms using the formula: PE =\[(Ip - Ia)/Ip\]\* 100%; based on an expected minimum effect size of 30%. First time infections in these subjects will offer relatively unambiguous evidence of the extent of exposure to infectious mosquito bites. The primary entomological endpoint will be adult densities of vector species via human-landing catch (HLC) from sentinel households from intervention and control arms over the follow-up period.

Secondary epidemiological endpoints will be the incidence density of first time malaria infections among human cohorts during the follow-up period as detected by microscopy and the total number of cases averted (i.e., all Plasmodium spp. infections in cohort subjects). Secondary entomological endpoints include number of sporozoite infected mosquitoes, parity and species-specific effects of the spatial repellent product.

Both epidemiological and entomological endpoints will be utilized to look at the relationship between SR and PE based on product coverage (to include diversion and community effects) and insect behavior. The prospect of SR associated temporal cumulative effects on study endpoints (epidemiological and entomological) over transmission seasons will also be investigated by using the cumulative incidence of infection over the season and applying a survival curve analysis of the cohort data.

Recruitment & Eligibility

Status
WITHDRAWN
Sex
All
Target Recruitment
Not specified
Inclusion Criteria
  • Children aged 6-59 months
  • glucose-6-phosphate dehydrogenase (G6PD) normal (qualitative screen) in sites where P. vivax or P. ovale known prevalence rates represent major burden) and whose treatment with primaquine is implemented within national guidelines
  • Hb > 5mg/dl
  • Temperature ≤38.0°C) and no moderate or severe acute illness/infection on the day of inclusion
  • Sleeps in cluster >90% of nights during any given month
  • No plans for extended travel (<1month) outside of home during study
  • Not participating in another clinical trial investigating a vaccine, drug, medical device, or a medical procedure during the trial
  • Provision of assent/informed consent form signed by the subject and by the parent(s) or another legally acceptable representative
Exclusion Criteria
  • children < 6 months or > 5 years
  • G6PD deficiency (qualitative screen) in sites where P. vivax or P. ovale known prevalence rates represent major burden and whose treatment with primaquine is implemented within national guidelines
  • Severe anemia
  • Febrile illness (temperature ≥38.0°C) or moderate or severe acute illness/infection on the day of inclusion
  • Sleeps in cluster <90% of nights during any given month
  • Plans for extended travel (>1month) outside of home during study
  • Participating or planned participation in another clinical trial investigating a vaccine, drug, medical device, or a medical procedure during the trial
  • No provision of assent/informed consent form signed by the subject and by the parent(s) or another legally acceptable representative

Study & Design

Study Type
INTERVENTIONAL
Study Design
PARALLEL
Arm && Interventions
GroupInterventionDescription
InterventionSpatial Repellent product with active ingredientSpatial Repellent product with active ingredient
InterventionActive ingredientSpatial Repellent product with active ingredient
PlaceboSpatial Repellent product without active ingredient (SHIELD)Placebo Repellent product with no active ingredient
Primary Outcome Measures
NameTimeMethod
Malaria Incidence104 weeks

Incidence of malaria infections among human cohorts during the follow-up period as detected by PCR

Secondary Outcome Measures
NameTimeMethod

Trial Locations

Locations (1)

Kemri-Crc

🇰🇪

Kisumu, Kenya

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