Age-based targeting of biannual azithromycin distribution for child survival in Niger: an adaptive cluster-randomized trial protocol (AVENIR)

AVENIR is a double-masked cluster-randomized placebo-controlled response-adaptive large simple trial in Niger. During a one-year run-in period, communities in the Dosso region in Niger will be randomized 1:1:1 to 1) azithromycin 1–11: biannual azithromycin to children 1–11 months old with placebo to children 12–59 months old, 2) azithromycin 1–59: biannual azithromycin to children 1–59 months old, or 3) placebo: biannual placebo to children 1–59 months old. Regions enrolled after the run-in period will be randomized with an allocation updated based on the probability of mortality in children 1–59 months in each arm during the preceding study period. Communities will retain their allocation for 4 distributions, after which they will be re-randomized with an updated allocation. All-cause mortality will be compared by arm at 2.5 years from the first enrollment. In a substudy, 50 randomly selected communities from each arm in the Dosso region will be followed to monitor antimicrobial resistance. Figure 1 summarizes the mortality and resistance trial designs for the Dosso and Tahoua regions.

The trial began enrollment in November 2020 and recruitment is anticipated through May 2023. Stage I includes enrollment through the primary mortality analysis and Stage II includes potential continued enrollment after this time point. This protocol adheres to the Standard Protocol Items: Recommendations for Interventional Trials (SPIRIT) guidelines (Supplementary Table S1, [21]) and refers to version 13 of the study protocol as revised 31 January 2021.

The objectives of this study are 1) to compare the efficacy of two age-based approaches to biannual mass azithromycin distribution to reduce all-cause mortality, 2) to compare selection for antimicrobial resistance across these strategies, and 3) to evaluate implementation-related outcomes, including the costs, feasibility, and acceptability of this intervention, and to compare these indicators across distribution strategies. Specifically, objective 1 has 3 aims: 1) to replicate and assess the generalizability of the MORDOR trial by comparing 1–59-month mortality in the azithromycin 1–59 and placebo arms, 2) to test the efficacy of targeting treatment to children 1–11 months old by comparing 1–11-month mortality in the azithromycin 1–11 and placebo arms, and 3) to determine the additional benefit of including older children by comparing 12–59-month mortality in the azithromycin 1–11 and azithromycin 1–59 arms. We hypothesize that mortality will be lower in both azithromycin arms compared to placebo, and lower in the azithromycin 1–59 arm compared to the azithromycin 1–11 arm at 2.5 years from the first enrollment. For objective 2, the aims are 1) to compare the community-level prevalence of genetic determinants of macrolide resistance in respiratory organisms across arms and 2) to compare the community-level load of genetic determinants of macrolide resistance in enteric organisms across arms. We hypothesize that, after 2 years of distributions, resistance will be higher in both azithromycin arms compared to placebo, and higher in the azithromycin 1–59 arm compared to azithromycin 1–11. Objective 3 involves the calculation of program costs for each strategy, analysis of the comparative cost-effectiveness, and the measurement of feasibility and acceptability as perceived by stakeholders at the community, implementer, and governmental levels. We hypothesize that the azithromycin 1–59 arm will be more cost-effective than the azithromycin 1–11 arm and that these strategies will be similarly feasible and acceptable.

Full eligibility criteria at the community and individual levels are described in Table 1. This study will include secure and accessible rural and peri-urban communities in the 5 regions of Niger with the largest under-5 populations (Dosso, Tahoua, Maradi, Zinder, Tillabéri; Fig. 2, Table 2), with Stage I targeting the Dosso, Tahoua, and the first half of the Maradi regions for inclusion. Dosso and Tahoua regions will contribute to the primary outcomes in Stage I. The estimated 2017 regional under-5 mortality rates were 116 per 1000 live births in Dosso, 101 in Tahoua, 110 in Maradi, 120 in Zinder, and 116 in Tillabéri [22]. We estimate that these 5 regions include approximately 14,630 eligible communities encompassing approximately 2.3 million eligible children under 5 (Table 2) and 3350 of these are targeted for inclusion in Stage I.

AVENIR was designed in collaboration with local, national, and global stakeholders in child health. Sensitization campaigns will be conducted at the community, district, regional, and national levels before study activities begin and leaders at these levels will continue to be engaged by the study team throughout the course of the trial and in the dissemination of results. All households will be recruited for participation in the census, and all children 1–59 months of age will be recruited for the intervention.

Implementation will be phased in by region (Fig. 2, Table 2). Communities in Dosso will be enrolled in the first year and randomized to the 3 arms in a 1:1:1 allocation. After 1 year, allocation probabilities for newly enrolled communities will adapt using the probability that each arm is superior with respect to the mortality rate in children 1–59 months, such that communities will have a higher probability of being allocated to the arm with the lowest mortality rate. From the pool of eligible communities in the Dosso region, a substudy will include a random sample of 50 communities per arm to monitor AMR outcomes.

After the primary outcome analysis at 2.5 years from the first enrollment, communities may be re-randomized with continued follow-up using the same adaptive allocation. To minimize the impact of a possible carry-over effect of treatment in the event that a community changes arms through adaptive allocation, each community will stay with its randomized assignment for 4 distributions (approximately 2 years). No community will be re-randomized by the time of the primary outcome analysis. Additional treatment arms may be added to the trial or arms may be dropped from the trial after the primary outcome analysis. With such changes, protocol details, power calculations, and analysis plans will be updated accordingly.

Masking will be facilitated by use of a matching placebo, which will be identical to azithromycin in appearance, smell, packaging, and distribution. Those masked to study arm allocation include participants, investigators, and most study personnel including census personnel administering treatment and collecting mortality outcomes and laboratory personnel processing samples for resistance outcomes. Unmasked personnel include the trial biostatistician and data analyst responsible for implementing the randomization sequence and key members of Pfizer staff responsible for implementation of the randomization sequence.

Azithromycin and placebo will be administered biannually as a single, directly observed dose of 20 mg/kg (up to the maximum adult dose of 1 g) as oral suspension using dosing cups or syringes. For children 1–11 months of age and those unable to stand, dose will be determined by weight using a hanging scale. For children 12–59 months of age able to stand, dose will be determined by height approximation as currently performed by Niger’s trachoma program [23]. Azithromycin and placebo will be prepared by Pfizer, Inc. (New York, NY, USA) and shipped directly to the study sites.

At the time of treatment, caregivers will be instructed to report any adverse event experienced by the treated child within 28 days of treatment to the study team. Serious adverse events will be reported to UCSF and the Medical Monitors within 24 h of notification, and to Pfizer, the Data and Safety Monitoring Committee (DSMC), and Institutional Review Boards (IRBs) according to the requirements of each. Children will be referred for follow-up care on a case-by-case basis.

All data will be collected electronically on mobile devices with a custom-designed mobile application (CommCare by Dimagi, Cambridge, MA, USA), and uploaded regularly to a secure, cloud-based server. All study personnel will attend intensive, two-day training sessions prior to conducting study procedures and collecting data. Data management teams in Niger and at UCSF will monitor data collection in real time daily. Investigators will visit study sites twice each year to monitor study implementation and ensure adherence to the study protocol.

Study participants will be assigned unique identification numbers that do not contain personal identifying information, which will be used to link data across databases and will be the only identifier shared in de-identified datasets. Upon completion of the trial, de-identified data will be made available upon request.

A Data and Safety Monitoring Committee (DSMC) will be empaneled before the study begins to provide independent oversight of data quality and participant safety. The DSMC will include independent experts with collective expertise in bioethics, biostatistics, antimicrobial resistance, and pediatric infectious disease. The DSMC will meet at least once per year to review study progress and adverse events, with ad hoc meetings convened as necessary. The DSMC will recommend modifications to the protocol as necessary. Major protocol changes will be reported to the DSMC and Institutional Review Board(s) as required.

Study investigators from UCSF and in Niger will monitor study conduct regularly through data monitoring as described above in addition to regular site visits to ensure adherence to the study protocol. Details of ethical approval and informed consent are included below. Two Medical Monitors with expertise in pediatrics and infectious disease will review the protocol before the trial begins and will review serious adverse events during the trial.