Treatment of Tuberculosis
ENDTB
endTB aims to find shorter, less toxic and more effective treatments for 'multidrug-resistant TB' (MDR-TB). In this randomized, controlled, open-label, multi-country Phase III trial, 5 experimental regimens containing 1 or 2 new drugs in patients with fluoroquinolone-susceptible MDR-TB are trailed. The objective is to assess whether the efficacy of experimental regimens at Week 73 is non-inferior to that of the control.
Countries
Georgia, India, Kazakhstan, Lesotho, Pakistan, Peru, South Africa, Vietnam
Tentative End date
April 2023
Our Role
Statistics & Data Management
For more information contact: Maelenn Gouillou
ENDTB-Q
ENDTB-Q is a randomized, controlled, open-label, multi-country Phase III trial (Randomization (2:1 in favor of the experimental arm) is stratified by country and extent-of-TB-disease phenotype). The objective is to Identify an effective, shorter, less toxic and injection-free regimen for FQ-resistant MDR-TB as compared to the current standard of care. The primary objective is to assess whether the efficacy of experimental 6 to 9 months regimen is non-inferior to that of the control at 73 weeks.
Countries
India, Kazakhstan, Lesotho, Pakistan, Peru, Vietnam
Tentative End date
April 2023
Our Role
Statistics & Data Management
For more information contact: Maelenn Gouillou
PANDRTB
PandrTB is a study of the pharmacokinetics (PK) and pharmacodynamics (PD) of bedaquiline, delamanid, clofazimine, linezolid, moxifloxacin, levofloxacin and pyrazinamide used in novel combinations to treat rifampicinresistant tuberculosis (RR-TB), including multidrug-resistant TB (MDR-TB), and fluoroquinolone-resistant TB (QR-TB). PandrTB is an observational study nested in the endTB and endTB-Q trials. The overarching aim is to estimate the PK and PD of the drugs as used in combination across the experimental arms of the endTB and endTB-Q trials.
Countries
Lesotho, Peru, South Africa, Pakistan
Tentative End date
April 2023
Our Role
Statistics & Data Management
For more information contact: Maelenn Gouillou
DATURA
For people with HIV associated severe immune suppression (CD4 ≤ 100 cells/ μL), TB incidence is high and represents the most frequent cause of hospitalization and death. In this study, "Determination of Adequate Tuberculosis Regimen in Adults and adolescents hospitalised with HIV associated severe immune suppression (CD4 ≤ 100 cells/μL)", we hypothesize that intensification of the initial phase of TB treatment, by increasing doses of two major TB drugs, rifampicin and isoniazid, and adding systematic corticosteroids, will decrease mortality in severely immunosuppressed HIVinfected adults and adolescents hospitalized for TB in comparison with the current standard TB regimen.
Objective
To estimate the impact of an intensified initial phase of Tuberculosis (TB) treatment on mortality at 48 weeks among HIVinfected adults and adolescents hospitalised for TB with CD4 ≤ 100 cells/μL in comparison with the standard TB regimen.
Methodology
A Phase III multicenter, two-arms, open-label randomised controlled superiority trial. Eligible subjects will be randomised in a 1:1 ratio for a total of 665 patients per trial arm, with stratification by country and by CD4 cell counts (≤ 50 or > 50 cells/μL).
Who's Involved Besides MSF?
Inserm - ANRS, EDCTP, Pathogenesis and Control of Chronic Infections (PCCI), UMR1058 (Inserm, University of Montpellier, EFS), Cambodia, Cameroon, Guinea, Uganda, Vietnam, Zambia
Country
Uganda
Tentative End date
December 2024
Our Role
Study Site
For more information contact: Gino Agbota
TB-SPEED
In 2017, an estimated 10M new cases and 1.6M deaths occurred due to tuberculosis (TB). Despite progress in reducing TB incidence and mortality in the past 20 years, TB is a top ten cause of death in children under 5 years worldwide, with 1,2M new cases and 230’000 deaths in 2019. The vast majority of children dying from TB are children (<5 years old) not accessing treatment, most likely because they are not diagnosed. The TB-Speed project will carry out research activities aiming at reducing childhood mortality.
Country
Uganda
Who's Invovled?
INSERM ; UNITAID ; Université de Bordeaux ; TB-Speed consotrium
TB-Speed HIV
A prospective multicentre study evaluating the safety & feasibility of the PAANTHER TB treatment decision algorithm for HIV-infected children with presumptive TB, conducted in 4 countries. The objective is to evaluate the safety of withholding TB treatment in HIV-infected children with presumptive TB not initiated on treatment as per the PAANTHER TB treatment-decision algorithm.
Tentative End date
December 2022
Our Role
Study Site
TB-Speed Pneumonia
A multicentric, cluster-randomised pragmatic diagnostic trial conducted in 5 countries, designed as a stepped wedge trial. The objective is to evaluate the impact on all-cause mortality at 12 weeks post inclusion of adding systematic early detection of TB with Ultra to the WHO-SOC in young children with severe pneumonia, followed by immediate anti-TB treatment initiation in children with a positive Ultra result, as compared to the SOC alone.
Tentative End date
December 2022
Our Role
Study Site
TB-Speed Decentralization
An observation phase followed by an intervention phase (randomisation of 2 districts per country between the 2 decentralization strategies). The objective is to assess the impact of a TB diagnostic approach decentralized at district hospital (DH) and Primary Health Care (PHC) levels on childhood TB case detection compared to the pre-intervention status and between 2 decentralized diagnostic strategies at DH and PHC levels.
Tentative End date
December 2022
Our Role
Study Site
TB-Speed Stool Processing
A diagnostic study evaluating the diagnostic accuracy of the Ultra assay in stools with a 2-stage sequential design starting as a cohort of children with presumptive TB enriched in a 2nd stage with Ultra positive TB cases on respiratory samples. The objective is to determine diagnostic accuracy of Xpert Ultra performed on stools processed using 4 different sample processing methods in children with presumptive TB.
Tentative End date
December 2022
Our Role
Study Site
For more information, contact
INTENSE TBM
The most lethal and disabling form of TB is TB meningitis (TBM), with an estimated 100,000 new cases occurring per year, representing around 6% of extra-pulmonary TB cases. In sub-saharan Africa, TBM mortality reaches 40% in HIV-negative patients and up to 70% in HIV-positive individuals with drug resistant M. tuberculosis (M. tb) strains. TBM treatment has remained unchanged for decades despite its relatively poor efficacy and there is not enough evidence that new anti-TB drugs becoming available could help manage TBM. In this study, "Intensified TB treatment with or without aspirin to reduce the mortality of HIVinfected and HIV-uninfected patients with tuberculous meningitis" we propose a treatment intensification of the first two months of anti-TB treatment based on high dose rifampicin (35 mg/kg/d orally) and Linézolide (4 weeks at 1200 mg/d and 4 weeks at 600mg/d), added to isoniazid, pyrazinamide and ethambutol at standard doses. The benefit of adding aspirin (200 mg/d) during the induction phase will be evaluated with and without intensified TB treatment. In addition, the study will allow us to gather data on the pharmacological interactions between high dose rifampicin and the new first line antiretroviral dolutegravir, and finally, on the incidence and risk factors of neurologic TB Immune Reconstitution Inflammatory syndrome.
Objective
Assess the efficacy of 2 interventions to reduce mortality from TBM with or without HIV coinfection in sub-Saharan Africa: Intensified TBM treatment compared to WHO standard TBM treatment ; Aspirin compared placebo.
Methodology
This is a randomized controlled, phase III, multicenter, 2 x 2 factorial plan superiority trial. The trial will be open-label for anti-TB treatment and placebo-controlled double blind for aspirin treatment.
Who’s Involved besides MSF?
Inserm-ANRS, EDCTP, MUST Uganda, Mbarara Regional Reference Hospital, Kabale Regional Referal Hospital, Intense TBM consortium:https://intense-tbm.org/
Country
Uganda
Tentative End date
December 2023
Our Role
Study Site