Azithromycin mass drug administration to reduce child mortality in Niger (AVENIR II): a master protocol for a cluster-randomized adaptive platform trial to evaluate community-based health interventions

  1. Ahmed M. Arzika
  2. Abdou Amza
  3. Sani Ousmane
  4. Ramatou Maliki
  5. Ibrahim Almou
  6. Nasser Galo
  7. Nasser Harouna
  8. Alio Mankara
  9. Bawa Aichatou
  10. Ousseini Boubacar
  11. Elodie Lebas
  12. Brittany Peterson
  13. Carolyn Brandt
  14. Andrea Picariello
  15. Angela Cheng
  16. Travis C. Porco
  17. Thuy Doan
  18. Benjamin F. Arnold
  19. Thomas M. Lietman
  20. Kieran S. O’Brien
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Abstract

Background

Trials have demonstrated that azithromycin mass drug administration (MDA) to children 1-59 months old reduces mortality, but increases antimicrobial resistance (AMR). The World Health Organization recommends that programs include mortality and AMR monitoring. Niger is expanding the azithromycin MDA for child survival program nationwide.

Methods

To establish program monitoring and leverage the infrastructure to evaluate other community health interventions, AVENIR II is designed as a cluster-randomized adaptive platform trial with monitoring and re-randomization every 2 years. The initial focus is to monitor under-5 mortality, AMR, implementation, and safety as the program expands in Niger. All eligible primary health center catchment areas (Centre de Santé Intégrés, CSIs) will be included in biannual oral azithromycin MDA to children 1-59 months old. A subset will be randomized to delay MDA for the first 2 years, after which they will receive MDA and another subset will be randomized to stop MDA for the next 2 years. The proportion randomized to delay or stop will be determined using an adaptive algorithm including: 1) results of prior azithromycin MDA mortality trials, 2) expert opinion on the appropriate ethical balance between delivering the program and monitoring AMR, and 3) statistical power to detect a programmatically relevant difference between arms. We anticipate 5-10% of CSIs will be randomized to delay or stop at each randomization. Mortality and AMR will be monitored at baseline and every 2 years. Implementation and safety outcomes will be monitored continuously. To enable ongoing monitoring while ensuring program access, CSIs receiving MDA will be re-randomized using the adaptive algorithm updated with new mortality results and no CSI will go without MDA for more than 2 years. In this platform design, additional arms may be added or dropped based on information from other studies, updates to guidelines, or preferences of Niger policymakers, and other interventions may be evaluated.

Discussion

The risk of AMR has led to caution in the implementation of azithromycin MDA. We present a design that enables continued rigorous evaluation of program impact on key outcomes, with flexibility to evaluate other interventions as well.

Trial registration

clinicaltrials.gov ( NCT06358872 ), registered April 2024

Article activity feed

  1. Version published to 10.1101/2025.06.17.25329431v1 on medRxiv