Effect of a participatory whole-systems approach on mortality in children younger than 5 years in Jigawa state, Nigeria (INSPIRING trial): a community-based, parallel-arm, pragmatic, cluster randomised controlled trial and concurrent mixed-methods process evaluation

In 2019, Nigeria reported the highest mortality rate in children younger than 5 years globally. We aimed to assess a whole-systems approach to improving child mortality in northern Nigeria. We conducted a community-based, parallel-arm, pragmatic, cluster randomised controlled trial in Kiyawa local g...

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Veröffentlicht in:The Lancet global health 2024-12, Vol.12 (12), p.e2035-e2048
Hauptverfasser: King, Carina, Burgess, Rochelle Ann, Bakare, Ayobami A, Shittu, Funmilayo, Salako, Julius, Bakare, Damola, Uchendu, Obioma C, Iuliano, Agnese, Djellouli, Nehla, Isah, Adamu, Haruna, Ibrahim, Ahmar, Samy, Ahmed, Tahlil, Valentine, Paula, Olowookere, Temitayo Folorunso, MacCalla, Matthew, Graham, Hamish R, McCollum, Eric D, Beard, James, Falade, Adegoke G, Colbourn, Tim, Bakare, Ayobami Adebayo, Cassar, Christine, Graham, Hamish G, Magama, Abdullahi, Olojede, Omotayo, Osebi, Adams, Seriki, Ibrahim, Sogbesan, Abiodun, Uchendu, Obioma
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Zusammenfassung:In 2019, Nigeria reported the highest mortality rate in children younger than 5 years globally. We aimed to assess a whole-systems approach to improving child mortality in northern Nigeria. We conducted a community-based, parallel-arm, pragmatic, cluster randomised controlled trial in Kiyawa local government area, Jigawa state, Nigeria, and a concurrent mixed-methods process evaluation using ethnography and quantitative implementation monitoring. Trial clusters were population catchment areas of 32 government primary health-care facilities. Compounds were randomly sampled, proportional to cluster size, and all women aged 16–49 years and children younger than 5 years who were permanent residents were eligible for inclusion and recruited as the evaluation population. Children younger than 7 days were recruited but excluded from analysis. Evaluation clusters were allocated to intervention or control via simple randomisation with a 1:1 ratio. Cluster names were written on paper, folded, and placed in a container by community representatives. Different community representatives took out names one by one, with the first half assigned to receive the intervention. The intervention consisted of three components: participatory learning and action (PLA) groups for men and women (including compound heads [ie, the member of the compound that residents deemed most senior]), partnership defined quality scorecard (PDQS), and health-care worker capacity building; it was delivered from March 1, 2021, to Dec 31, 2022. We could not mask participants, field staff, or intervention-delivery staff to cluster allocation but baseline, endline, and follow-up data excluded information on cluster allocation. PLA groups involved separate groups of up to 25 men or women from all villages in the intervention clusters. The primary outcome was all-cause mortality in children aged 7 days to 59 months between Oct 1, 2021, and Sept 20, 2022, referred to as the evaluation period. The trial was prospectively registered (ISRCTN 39213655) and the protocol has been published. We recruited 3800 compounds at baseline, with 12 893 children contributing to analysis of the primary outcome (7316 [56·8%] of 12 893 in the intervention group and 5577 [43·3%] in the control group). 6617 (51·3%) of 12 893 children were male, 6275 (48·7%) were female, and one (
ISSN:2214-109X
2214-109X
DOI:10.1016/S2214-109X(24)00369-3