The NICE-GUT trial protocol: A randomised, placebo controlled trial of oral nitazoxanide for the empiric treatment of acute gastroenteritis among Australian Aboriginal children

Waddington, CS; Mcleod, C; Morris, P; Bowen, A; Naunton, M; Carapetis, J; Grimwood, K; Robins-Browne, R; Kirkwood, Carl D; Baird, R; Green, D; Andrews, R; Fearon, D; Francis, J; Marsh, JA; Snelling, T

doi:10.26181/60c95cbce399e

The NICE-GUT trial protocol: A randomised, placebo controlled trial of oral nitazoxanide for the empiric treatment of acute gastroenteritis among Australian Aboriginal children

journal contribution

posted on 2021-06-16, 02:06 authored by CS Waddington, C Mcleod, P Morris, A Bowen, M Naunton, J Carapetis, K Grimwood, R Robins-Browne, Carl D Kirkwood, R Baird, D Green, R Andrews, D Fearon, J Francis, JA Marsh, T Snelling

Introduction Diarrhoeal disease is the second leading cause of death in children under 5 years globally, killing 525 000 annually. Australian Aboriginal and Torres Strait Islander (hereafter Aboriginal) children suffer a high burden of disease. Randomised trials in other populations suggest nitazoxanide accelerates recovery for children with Giardia, amoebiasis, Cryptosporidium, Rotavirus and Norovirus gastroenteritis, as well as in cases where no enteropathogens are found. Methods and analysis This double blind, 1:1 randomised, placebo controlled trial is investigating the impact of oral nitazoxanide on acute gastroenteritis in hospitalised Australian Aboriginal children aged 3 months to <5 years. Dosing is based on age-based dosing. The primary endpoint is the time to resolution of€significant illness' defined as the time from randomisation to the time of clinical assessment as medically ready for discharge, or to the time of actual discharge from hospital, whichever occurs first. Secondary endpoints include duration of hospitalisation, symptom severity during the period of significant illness and following treatment, duration of rehydration and drug safety. Patients will be followed for medically significant events for 60 days. Analysis is based on Bayesian inference. Subgroup analysis will occur by pathogen type (bacteria, virus or parasite), rotavirus vaccination status, age and illness severity. Ethics and dissemination Ethics approval has been granted by the Central Australian Human Research Ethics Committee (HREC-14-221) and the Human Research Ethics Committee of the Northern Territory Department of Health and Menzies School of Health Research (HREC2014-2172). Study investigators will ensure that the trial is conducted in accordance with the principles of the Declaration of Helsinki. Individual participant consent will be obtained. Results will be disseminated via peer-reviewed publication.

Funding

This work was supported by The National Health Medical Research Council (1069772). Fellowship support was provided by The National Health Medical Research Council (111657 and 1088735) and the Channel 7 Telethon Foundation.

History

Publication Date

2018-01-01

Journal

BMJ Open

Volume

8

Issue

2

Article Number

e019632

Pagination

8p. (p. 1-8)

Publisher

BMJ Group

ISSN

2044-6055

Rights Statement

The Author reserves all moral rights over the deposited text and must be credited if any re-use occurs. Documents deposited in OPAL are the Open Access versions of outputs published elsewhere. Changes resulting from the publishing process may therefore not be reflected in this document. The final published version may be obtained via the publisher’s DOI. Please note that additional copyright and access restrictions may apply to the published version.