Malaria Clinical Trial
Official title:
Evaluation of the Effect of Targeted Mass Drug Administration and Reactive Case Detection on Malaria Transmission and Elimination in East Hararghe Zone, Oromia, Ethiopia
NCT number | NCT04241705 |
Other study ID # | 1 |
Secondary ID | |
Status | Recruiting |
Phase | N/A |
First received | |
Last updated | |
Start date | January 20, 2020 |
Est. completion date | January 20, 2022 |
Reactive and proactive case detection measures are widely implemented by national malaria elimination programs globally. Similarly, the Ethiopian Federal Ministry of Health decided to include reactive case detection (RCD) and targeted mass drug administration (tMDA) approaches as part of their elimination strategy, along with rigorous evaluation. This study aims to evaluate the impact on annual parasite incidence (API) and cost-effectiveness of implementing tMDA and RCD within a 100-meter radius of passively detected index case, compared with standard of care in the control arm. In addition, cross-sectional surveys will measure the change in malaria prevalence over the two-year study intervention period. The aim is to generate evidence to inform Ethiopia's national strategy for malaria elimination.
Status | Recruiting |
Enrollment | 48960 |
Est. completion date | January 20, 2022 |
Est. primary completion date | January 20, 2022 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 6 Months and older |
Eligibility |
Inclusion Criteria: - Woreda-level: Of the 19 woredas with malaria risk, the ten woredas with the highest annual parasite incidence (API) in 2018 will be eligible for the study. - For Kebeles: - Kebeles in East Hararghe Zone targeted for implementation of elimination activities by the Ethiopian Federal Ministry of Health where there is ongoing PMI-supported malaria surveillance; - Kebeles with reported API between 1 and 50; - Kebeles in malarious districts with comparable optimization of malaria control interventions. - For individual participants: - All residents of the intervention study kebeles diagnosed with malaria at health facilities (index case) or reside within 100-meter radius with the index case and has NONE of the exclusion criteria listed below - Able to provide informed written consent Exclusion Criteria: - For kebeles: Kebeles planning on starting for the first time or discontinuing indoor residual spraying (IRS) campaigns in the next two years. - For individual participants: - Children less than 6 months of age or <5 kg - Known allergy or history of adverse reaction or chronic/congenital disease contra indicated to any of the intervention drugs: PQ, AL or CQ - Individuals with severe malnutrition or signs of severe disease, with evidence of any organ failure or Hgb level < 8gm/dl - Household members already covered by the intervention less or equal to one month before In addition, the following individuals will be excluded from receiving primaquine: - Phenotypically G6PD deficient individuals - Pregnant women - Lactating women breastfeeding infants less than 6 months of age or with unknown G6PD status |
Country | Name | City | State |
---|---|---|---|
Ethiopia | Woreda 6: | Alemaya | |
Ethiopia | Woreda 1: | Babile | |
Ethiopia | Woreda 2: | Fedis | |
Ethiopia | Woreda 3: | Girawa | |
Ethiopia | Woreda 4: | Golo oda | |
Ethiopia | Woreda 5: | Gursum | |
Ethiopia | Woreda 7: | Kersa | |
Ethiopia | Woreda 8: | Kombolcha | |
Ethiopia | Woreda 9: | Kurfa chele | |
Ethiopia | Woreda 10: | Midega Tola |
Lead Sponsor | Collaborator |
---|---|
Armauer Hansen Research Institute, Ethiopia | Addis Continental Institute of Public Health, Ethiopian Federal Ministry of Health, Oromia Regional Health Bureau, Tulane University, U.S. Centers for Disease Control and Prevention, U.S. President's Malaria Initiative, United States Agency for International Development (USAID) |
Ethiopia,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Change in malaria annual parasite incidence (API) | The effect of RCD or tMDA will be defined as a change in malaria API among residents measured by microscopy/RDT through health centers and health posts. The malaria API will be defined as all passively detected RDT or microscopy confirmed cases over a period of 12 months, who are residents of the kebele divided by the estimated population in the intervention kebele multiplied by 1000. The primary effectiveness endpoint will therefore be API among residents of the kebele at baseline and year 2 of each intervention group of study clusters, compared with the control clusters. | Two years | |
Secondary | Malaria burden, measured by antigen test | Testing for pan-Plasmodium antigens aldolase and LDH will determine active infection with malaria parasite, and, if the infecting species is Pf, by the presence of HRP2 antigen (Plucinski, Herman et al. 2018). | Two years | |
Secondary | Malaria burden, measured by serology | Sero-prevalence will be determined using LUMINEX based multiplex assays. Age-specific sero-conversion and sero-reversion rates over the two years will be used to monitor changes in transmission and malaria exposure over time. Absence of antimalarial antibodies, particularly in children, will show the success of tMDA or RCD interventions. Antigen selection will be informed by recent studies by EPHI and CDC and a panel of antibodies characterized to indicate recent change in transmission will be included (Kerkhof, Sluydts et al. 2016). | Two years | |
Secondary | Malaria burden, measured by molecular testing | Real-time quantitative (qPCR) for parasite detection will be performed by targeting the 18S small rRNA gene for Pf and Pv using primer and probe sequences. Pf parasites will be quantified using standard curves generated from a serial dilution of NF54 ring stage parasites. Pv parasite quantification will be done using plasmid constructs to infer copy numbers as described before. Blood samples in RNA protect buffers will be used for extraction of RNA using the RNeasy Mini Kit (QIAGEN) for gametocyte quantification, gametocyte commitment and maturation assays, sex ratio estimation, asexual stage parasites detection, and expression level of regulators of the balance between reproduction and replication. | Two years | |
Secondary | Intervention coverage | To compare intervention coverage in RCD and tMDA arms. After RCD and tMDA interventions, coverage will be estimated by calculating the proportion of all enumerated household members reached in each index case event and the proportion of individuals tested and/or on treatment. | Two years | |
Secondary | Acceptability | To compare acceptability of RCD and tMDA. During the baseline and endline cross-sectional surveys, the household head will be asked questions about the acceptability of the RCD and tMDA interventions (self-report). | Two years | |
Secondary | Serious adverse events | To compare number of serious adverse events between the RCD and tMDA arms | Two years | |
Secondary | Adherence | To compare the adherence to antimalarials between the RCD and tMDA arms. Adherence will be measured by self-report and pill count. | Two years | |
Secondary | Costs | To compare the costs of RCD and tMDA. Costs will be calculated using an ingredients approach that involves enumerating both the quantity of specific inputs (e.g., hours spent, cost of treatment, number of RDTs used, etc.) and the time spent during the intervention. Quantity and time will be converted to a common monetary cost measure. Existing infrastructure and recurrent inputs that would be present in the absence of the intervention will not be included in cost analysis. The emphasis of the cost analysis is on determining the cost of RCD and tMDA alone. | Two years | |
Secondary | Cost-effectiveness | To assess the cost-effectiveness of RCD and tMDA relative to control. Cost-effectiveness will be measured through incident malaria cases averted as measured through the difference in malaria incidence in RCD and tMDA kebeles. | Two years | |
Secondary | Sensitivity and specificity of polymerase chain reaction (PCR) | To evaluate the sensitivity and specificity of PCR as compared to antigen- based multiplex testing | Two years | |
Secondary | Ratio of imported to locally acquired incident cases | To assess the ratio of imported to locally acquired incident cases | Two years |
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