Levofloxacin versus placebo for the prevention of tuberculosis disease in child contacts of multidrug-resistant tuberculosis: study protocol for a phase III cluster randomised controlled trial (TB-CHAMP)

James A Seddon,Lee Fairlie,Angela M Crook,Anne-Marie Demers,Graeme Hoddinott,Ellen Owen-Powell,Anneke C Hesseling,Anthony J Garcia-Prats,Muhammad Osman,Anna Turkova,H Simon Schaaf,Susan E Purchase,Diana M Gibb,Margaret J Thomason,Neil Martinson

doi:10.1186/s13063-018-3070-0

Abstract

BackgroundMultidrug-resistant (MDR) tuberculosis (TB) presents a challenge for global TB control. Treating individuals with MDR-TB infection to prevent progression to disease could be an effective public health strategy. Young children are at high risk of developing TB disease following infection and are commonly infected by an adult in their household. Identifying young children with household exposure to MDR-TB and providing them with MDR-TB preventive therapy could reduce the risk of disease progression. To date, no trials of MDR-TB preventive therapy have been completed and World Health Organization guidelines suggest close observation with no active treatment.MethodsThe tuberculosis child multidrug-resistant preventive therapy (TB-CHAMP) trial is a phase III cluster randomised placebo-controlled trial to assess the efficacy of levofloxacin in young child contacts of MDR-TB cases. The trial is taking place at three sites in South Africa where adults with MDR-TB are identified. If a child aged < 5 years lives in their household, we assess the adult index case, screen all household members for TB disease and evaluate any child aged < 5 years for trial eligibility. Eligible children are randomised by household to receive daily levofloxacin (15–20 mg/kg) or matching placebo for six months. Children are closely monitored for disease development, drug tolerability and adverse events. The primary endpoint is incident TB disease or TB death by one year after recruitment. We will enrol 1556 children from approximately 778 households with an average of two eligible children per household. Recruitment will run for 18–24 months with all children followed for 18 months after treatment. Qualitative and health economic evaluations are embedded in the trial.DiscussionIf the TB-CHAMP trial demonstrates that levofloxacin is effective in preventing TB disease in young children who have been exposed to MDR-TB and that it is safe, well tolerated, acceptable and cost-effective, we would expect that that this intervention would rapidly transfer into policy.Trial registrationISRCTN Registry, ISRCTN92634082. Registered on 31 March 2016.

Highlights

Multidrug-resistant (MDR) tuberculosis (TB) presents a challenge for global TB control
Modelling suggests that two million children are currently living with MDR-TB infection [4] and of the children infected with M. tuberculosis who progress to disease, 90% will do so within 12 months [5]
Trial design The tuberculosis child multidrug-resistant preventive therapy (TB-CHAMP) trial is a phase III cluster randomised placebo-controlled trial to assess the efficacy of levofloxacin to prevent TB disease in young child contacts of people with MDR-TB disease

Summary

Methods

Trial design The tuberculosis child multidrug-resistant preventive therapy (TB-CHAMP) trial is a phase III cluster randomised placebo-controlled trial to assess the efficacy of levofloxacin to prevent TB disease in young (aged < 5 years) child contacts of people with MDR-TB disease. We plan to adapt the trial design to include delamanid to treat child contacts of fluoroquinolone-resistant MDR-TB, in an observational cohort, once pharmacokinetic data and formulations become available for the youngest children, dependent on additional funding. Choice of control regimen As outlined above, isoniazid may be active against M. tuberculosis with inhA promoter region mutations, as well as susceptible strains from exposures other than the identified index case For these reasons, the PHOENIx randomised controlled trial (A5300/IMPAACT2003), evaluating MDRTB infection treatment with delamanid, chose isoniazid for their control arm. As stated above, we anticipate high concordance between index case and child contact (with few children infected with drug-susceptible strains), as well as globally limited utility of isoniazid to treat MDR strains (due to the preponderance of katG gene mutations worldwide). Child aged < 5 years who is a household contact of an enrolled adult MDR-TB index case diagnosed during the previous 6 monthsb

Discussion

Background

TB disease at enrolment

Findings