An open-label, randomized, non-inferiority trial of the efficacy and safety of ciprofloxacin versus an aminoglycoside + ciprofloxacin in the treatment of bubonic plague (IMASOY): study protocol for a randomized control trial—an update to the published protocol

This article reports an update to the protocol of the IMASOY trial, which was prospectively registered on clinicaltrials.gov (NCT04110340) in October 2019.

Observational non-comparative study of pneumonic plague

In 2021, new treatment guidelines were released by the US Centers for Disease Control and Prevention that recommend the use of a combination therapy for pneumonic plague. As no clinical equipoise exists to demonstrate a potential benefit of a monotherapy to treat pneumonic plague, it was therefore considered to be unethical to continue randomizing patients with suspected pneumonic plague to receive a monotherapy (ciprofloxacin alone). Patients with pneumonic plague symptoms at admission were therefore enrolled to an observational cohort and the outcomes of the current standard of care treatment (as per the national treatment guidelines) will be reported. Note: patients who are admitted and enrolled with suspected bubonic plague and who later develop pneumonic plague will remain in the randomized cohort, receive appropriate treatment for pneumonic plague as per national treatment guidelines and will be treated as a treatment failure.

Exploratory objectives

Three exploratory objectives were removed from the protocol. The analysis will not include the following: comparison of different methods for detection of anti-Yersinia pestis antibodies; measurement of the performance of qPCR for plague diagnosis; evaluation of new rapid tests.

Case definitions

The case definition (Table 1) has been modified in line with the revised international plague case definition (2021) [2].

Control arm

Due to the expiration of the national supply of streptomycin in Madagascar and lack of global availability of new stock, the control arm treatment was amended from streptomycin + ciprofloxacin to an aminoglycoside + ciprofloxacin. Under Madagascar’s national treatment guidelines for bubonic plague, gentamicin is the next alternative aminoglycoside treatment option. To account for treatment heterogeneity in the control arm, a sensitivity analysis will be planned as part of the final analysis.

Primary endpoint

Following the publication of the results of a study evaluating the precision and intra-rater agreement of the measurement of artificial buboes using a digital calliper [3], it was agreed that the measurement of artificial buboes with a digital calliper is unreliable and raised concerns about the potential impact of significant measurement error on the assessment of the composite primary endpoint of the IMASOY trial—a component of which requires detection of a 25% reduction in bubo size. The primary endpoint was therefore amended to remove component evaluating bubo size. The original composite endpoint was retained as a new secondary endpoint.

Schedule of events

A trial visit was added at M12 (± 2-month window) for patients who return a positive antibody (IgM or IgG) test at M3.

The IMASOY closed to recruitment in March 2024 having recruited over 220 probable and confirmed cases of bubonic plague—the planned minimum sample size was 190. The trial results will be available in Q4 of 2024.

Not applicable—no data have been collected as part of this publication.

Not applicable.

This trial is supported by the Foreign Commonwealth and Development Office and Wellcome [216273/Z/19/Z]. The role of the funder is to provide financial support for the trial. The trial collaborators are responsible for the design, management and analysis of the trial and the publication of the trial results.

Authors and Affiliations

1. Institut Pasteur de Madagascar, Antananarivo, Madagascar

   Rindra Vatosoa Randremanana, Gabriella Zadonirina, Hanitra Razananaivo, Théodora Mayouya-Gamana, Reziky Mangahasimbola, Minoarisoa Rajerison & Voahangy Andrianaivoarimanana

2. Centre d’Infectiologie Charles Mérieux, University of Antananarivo, Antananarivo, Madagascar

   Mihaja Raberahona

3. Department of Infectious Diseases, University Hospital Joseph Raseta Befelatanana, Antananarivo, Madagascar

   Mihaja Raberahona & Mamy Jean de Dieu Randria

4. Faculty of Medicine, University of Antananarivo, Antananarivo, Madagascar

   Mamy Jean de Dieu Randria

5. ISARIC, Pandemic Sciences Institute, University of Oxford, Oxford, UK

   Josephine Bourner, Elise Pesonel, Annelies Gillesen, Peter Horby & Piero Olliaro

6. London School of Hygiene and Tropical Medicine, London, UK

   Tansy Edwards

Contributions

This article was written by JB and based on the amended trial protocol written by RR, MR, JB, GZ, HR, TMG, EP, TE, PO and PH. All authors have approved the submitted manuscript.

Corresponding author

Correspondence to Josephine Bourner.

Ethics approval and consent to participate

This study has been conducted in accordance with the Declaration of Helsinki and the applicable principles of the International Committee on Harmonization of Good Clinical Practice (GCP-ICH). The protocol, the informed consent form and the CRF (and their respective amendments) have received approval from the Madagascar Biomedical Research Ethics Committee (ref: 116/MSANP/SG/AGMED/CERBM), and the protocol, patient information sheet and informed consent form (and their respective amendments) have received approval from the Oxford Tropical Research Ethics Committee and the Ethics Committee (ref: 45–18) of the London School of Hygiene and Tropical Medicine (ref: 17911). Written informed consent to participate will be obtained from all participants.

Consent for publication

Not applicable—no details, images or videos relating to an individual person have been collected as part of this publication.

Competing interests

The authors declare they have no competing interests.

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