Pneumonia Clinical Trial
— TIMCIOfficial title:
Tools for the Integrated Management of Childhood Illness: Evaluation of Pulse Oximetry and Clinical Decision Support Algorithms in Primary Care. Cross-country Quasi-experimental Pre-post Study, With Embedded Mixed Methods Studies, Cost and Modelled Cost-effectiveness in Kenya and Senegal
NCT number | NCT05065320 |
Other study ID # | ERC.0003406 |
Secondary ID | |
Status | Completed |
Phase | |
First received | |
Last updated | |
Start date | August 16, 2021 |
Est. completion date | March 31, 2023 |
Verified date | November 2022 |
Source | Swiss Tropical & Public Health Institute |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Observational [Patient Registry] |
By introducing pulse oximetry, with or without clinical decision support algorithms, to primary care facilities in India, Kenya, Senegal and Tanzania, the Tools for Integrated Management of Childhood Illness (TIMCI) project aims to contribute to reducing morbidity and mortality for sick children under-five while supporting the rational and efficient use of diagnostics and medicines by healthcare providers. The multi-country, multi-method evaluation aims to generate evidence on the health and quality of care impact, operational priorities, cost and cost-effectiveness of introducing these tools to facilitate national and international decision-making on scale-up.
Status | Completed |
Enrollment | 51590 |
Est. completion date | March 31, 2023 |
Est. primary completion date | March 31, 2023 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | 1 Day to 5 Years |
Eligibility | Inclusion Criteria: - Children 0-59 months of age for whom caregivers provide consent - Consulting for an illness, or reported to be unwell when attending for a routine visit (e.g. vaccination, growth or chronic disease monitoring) Exclusion Criteria: - Children in the immediate post-natal period or first day of life - Attending for a consultation related to trauma only (including new and follow-up presentations for burns, injuries, wounds) - Admitted within an inpatient part of the facility (including neonates delivered at the facility admitted with their mother) - Enrolled in the study within the preceding 28 days at any study facility |
Country | Name | City | State |
---|---|---|---|
Kenya | University of Nairobi | Nairobi | |
Senegal | UCAD | Dakar |
Lead Sponsor | Collaborator |
---|---|
Swiss Tropical & Public Health Institute | Burnet Institute, Cheikh Anta Diop University, Senegal, PATH, University of Nairobi |
Kenya, Senegal,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Proportion of children referred by a primary care healthcare provider to a higher level of care (either to a hospital or to an inpatient part of a larger primary healthcare facility) at Day 0 consultation | The denominator will be all children recruited. Only urgent referrals will be considered. | At time of enrolment | |
Primary | Proportion of children prescribed an antibiotic at Day 0 | Only antibacterials for systemic use will be taken into account for the definition of antibiotics. All children recruited will be counted in the denominator. | At time of enrolment | |
Secondary | Proportion of children with a severe complication (death or secondary hospitalisation) by Day 7 | Secondary hospitalisation refers to any delayed hospitalisation (occurring at any point greater than 24 hours after Day 0 consultation) and any hospitalisation occurring without referral. The denominator is all enrolled children.. | From enrolment up to 7 days after | |
Secondary | Proportion of children admitted to hospital within 24 hours of the Day 0 primary care consultation and as a result of a referral | This is used as a proxy for 'appropriate referral' of children, as those with severe disease should generally be admitted to hospital. The denominator for this outcome is also all children enrolled in the study, rather than only referred children. This is because the proportion of referred children that are admitted may be high in routine care, in the context of an inappropriately low referral rate. The aim of the intervention is therefore to increase the overall referral rate of children with severe disease. Hospital admission is chosen as the proxy of severe disease rather than using primary care classification of severe disease, as there are inadequacies in the classification of severe disease in routine practice. A child will be considered admitted to hospital 24hrs of Day0 consultation if the date of hospitalization is the same as Day0 date or is one day after Day0 date. | From enrolment up to 1 day after | |
Secondary | Proportion of children who completed referral, as reported at day 7 follow-up | Only urgent referrals will be considered. A referral will be considered completed if a child attended a hospital, whether was admitted or not. A window of +3 days from Day 7 is considered. | From enrolment up to 10 days after | |
Secondary | Proportion of children cured (defined as caregiver reported recovery from illness) by Day 7 | The denominator will be all children recruited. A window of +3 days from Day 7 is considered. | From enrolment up to 10 days after | |
Secondary | Proportion of children with non-severe disease referred to a higher level of care on Day 0 | Only urgent referrals will be considered. Only urgent referrals will be considered. | At time of enrolment | |
Secondary | Average length of stay (in days) of children admitted to hospital | If a child is hospitalised twice, the first hospitalization will be used and second hospitalizations will be reported separately. The denominator will be all hospitalised children. This is not a time-to-event outcome measure, as it will be analysed as a continuous variable. | From hospital admission to discharge | |
Secondary | Proportion of children prescribed a diagnosis-appropriate antibiotic | Appropriateness of antibiotic prescription in relation to diagnosis will be evaluated as:
diagnosis for which a systemic antibiotic was indicated and a systemic antibiotic was prescribed diagnosis for which a systemic antibiotic was not indicated and systemic antibiotic was prescribed first-line (or second-line) antibiotics were prescribed according to recommendations for IMCI diagnoses for which specific antibiotic(s)are indicated Diagnoses will be classified according to whether systemic antibiotics are indicated, based on IMCI and other relevant national guidelines as used for the CDSA. |
At time of enrolment | |
Secondary | Proportion of febrile children tested for malaria at Day 0 | A child will be considered to be febrile if history of fever was reported by the caregiver before the consultation or temperature was recorded to be above or equal 37.5 C°. Only febrile children will be counted in the denominator. | At time of enrolment | |
Secondary | Proportion of malaria positive children prescribed an antimalarial | Only children with a positive malaria test result will be counted in the denominator. | At time of enrolment | |
Secondary | Proportion of malaria negative children prescribed an antimalarial | Only children with a negative malaria test result will be counted in the denominator. | At time of enrolment | |
Secondary | Proportion of untested children prescribed an antimalarial | Only children untested for malaria will be counted in the denominator. | At time of enrolment | |
Secondary | Proportion of children with severe, moderate and mild hypoxaemia, adjusted for sites at high altitude | The following SpO2 values ranges will be used: SpO2 < 90%, 90% = SpO2 < 92% and 92% = SpO2 < 94%. All children recruited will be in the denominator. | At time of enrolment | |
Secondary | Proportion of children with hypoxaemia (according to differing cut-offs) with severe complication | The following SpO2 values ranges will be used: SpO2 < 90%, 90% = SpO2 < 92% and 92% = SpO2 < 94%, spurious values and missing values. Each SpO2 group will be the denominator of each proportion. | At time of enrolment | |
Secondary | Proportion of children with severe hypoxaemia not meeting any other clinical criteria for severe disease | Country's specific cut-off for severe hypoxaemia will be used. All children recruited will be in the denominator. | At time of enrolment | |
Secondary | Proportion of children referred with hypoxaemia who receive oxygen at hospital | All children recruited will be in the denominator. Referral and hypoxaemia are assessed at Day0 consultation. Oxygen use at hospital is only available for hospitalised children from hospital records. At the time of enrolment hypoxaemia is measured and referral advise might be issued. Whether the child received oxygen or not at hospital is evaluated based on hospital registry and it refers to oxygen given at arrival to hospital. The specified time frame takes into account that the outcome is evaluated considering information recorded at different time points. | At time of enrolment and at time of hospitalization | |
Secondary | Proportion of children attending scheduled follow-up at the same facility by Day 7 | All children recruited will be in the denominator. | From enrolment up to 7 days after | |
Secondary | Proportion of children presenting for unscheduled follow-up to any health facility by Day 7 | All children recruited will be in the denominator. | From enrolment up to 7 days after |
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