Tri-Do-Re: Novel Triple-dose Tuberculosis Retreatment Regimen

Sponsor

Institute of Tropical Medicine, Belgium (Other)

Overall Status

Recruiting

CT.gov ID

NCT04260477

Collaborator

Damien Foundation (Other)

370

Enrollment

Location

Arms

44.1

Anticipated Duration (Months)

8.4

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

To determine if a high-dose first-line regimen is non-inferior (non-inferiority margin 10%) in terms of safety to the same regimen at regular dosing, in previously treated patients with rifampicin-susceptible recurrent Tuberculosis (TB).

Condition or Disease	Intervention/Treatment	Phase
Multidrug-resistant Tuberculosis Pulmonary Tuberculosis Tuberculosis Resistance to Tuberculostatic Drugs	Drug: 6EH³R³Z Drug: 6EHRZ	Phase 3

Detailed Description

This is a pragmatic open-label multi-stage randomized clinical trial. Potential participants will be screened and enrolled in Damien Foundation (DF) clinics participating in the trial.

First we will perform a two-arm study with 6EHRZ as control arm and 6EH³R³Z as intervention arm. If at interim analysis the intervention arm is not considered to be non-inferior to the control arm, the intervention stops and enrolment will continue in a an adapted intervention arm and the control arm (6EHRZ). Otherwise, enrolment continues to 6EHRZ and 6EH³R³Z.

As per routine practice, during treatment patients are in daily contact with the direct observed therapy (DOT) supervisor and minimally monthly clinic visits are scheduled for monitoring of safety and treatment response.

Additionally, liver function tests will be performed at fixed intervals during treatment. Six month and one year after treatment completion or cure the patient will be checked for relapse with systematic sputum acid-fast bacilli (AFB)-microscopy and TB culture.

Study Design

Study Type:

Interventional

Anticipated Enrollment :

370 participants

Allocation:

Randomized

Intervention Model:

Parallel Assignment

Masking:

None (Open Label)

Masking Description:

Providers in the TB clinics and lab technicians in the Niger clinics and labs will not be blinded to the prescribed regimen. However, lab technicians working in the Institute of Tropical Medicine (ITM) lab will be blinded to the prescribed regimen. Also the statistician will be blinded to the prescribed regimen until the first interim analysis is completed.

Primary Purpose:

Treatment

Official Title:

Novel Triple-dose Tuberculosis Retreatment Regimen: How to Overcome Resistance Without Creating More in Niger

Actual Study Start Date :

Mar 1, 2021

Anticipated Primary Completion Date :

Nov 1, 2024

Anticipated Study Completion Date :

Nov 1, 2024

Arms and Interventions

Arm	Intervention/Treatment
Experimental: 6EH³R3Z (Rifampicin (R)/ Isoniazid (H) / Pyrazinamide (Z)/Ethambutol (E)) 6-month high-dose treatment; New high-dose isoniazid / high-dose rifampicin retreatment regimen (6EH³R3Z) - that includes triple-dose rifampicin (R3; 30 mg/kg), and triple-dose isoniazid (H3; 15 mg/kg), complemented with pyrazinamide (Z) and ethambutol (E).	Drug: 6EH³R³Z A triple dose is defined as the triple of the routine dose used for a specific WHO weight band. Hence, the mg/kg within a weigh-band varies, as is the case in routine practice. Dosing takings into consideration the fixed dose combination (FDC) tablets (one tablet: 150 mg R + 75 mg H + 400 mg Z + 275mg E). Dosage relies on tables with dosage by weight-bands used by WHO for the Cat. 1 regimen. The dosage used for the intensive phase of the Cat. 1 regimen applies for the whole treatment duration. A double dose of H and R is added to the recommended normal dose for adults (WHO,2003) Other Names: Ethambutol; isoniazid; rifampicin; pyrazinamide triple dose isoniazid triple dose rifampicin
Active Comparator: 6EHRZ Standard of care: 6-month 6RHZE regimen with dose combination tablets (one tablet: 150 mg R + 75 mg H + 400 mg Z + 275mg E)	Drug: 6EHRZ Recommended normal dose adults (WHO, 2003) H: 5 (4-6) mg/kg/day R: 10 (8-12) mg/kg/day Z: 25 (20-30)mg/kg/day E: 15 (15-18)mg/kg/day Other Names: Ethambutol; isoniazid; rifampicin; pyrazinamide

Arm

Intervention/Treatment

Experimental: 6EH³R3Z

(Rifampicin (R)/ Isoniazid (H) / Pyrazinamide (Z)/Ethambutol (E)) 6-month high-dose treatment; New high-dose isoniazid / high-dose rifampicin retreatment regimen (6EH³R3Z) - that includes triple-dose rifampicin (R3; 30 mg/kg), and triple-dose isoniazid (H3; 15 mg/kg), complemented with pyrazinamide (Z) and ethambutol (E).

Drug: 6EH³R³Z

A triple dose is defined as the triple of the routine dose used for a specific WHO weight band. Hence, the mg/kg within a weigh-band varies, as is the case in routine practice. Dosing takings into consideration the fixed dose combination (FDC) tablets (one tablet: 150 mg R + 75 mg H + 400 mg Z + 275mg E). Dosage relies on tables with dosage by weight-bands used by WHO for the Cat. 1 regimen. The dosage used for the intensive phase of the Cat. 1 regimen applies for the whole treatment duration. A double dose of H and R is added to the recommended normal dose for adults (WHO,2003)

Other Names:

Ethambutol; isoniazid; rifampicin; pyrazinamide

triple dose isoniazid

triple dose rifampicin

Active Comparator: 6EHRZ

Standard of care: 6-month 6RHZE regimen with dose combination tablets (one tablet: 150 mg R + 75 mg H + 400 mg Z + 275mg E)

Drug: 6EHRZ

Recommended normal dose adults (WHO, 2003) H: 5 (4-6) mg/kg/day R: 10 (8-12) mg/kg/day Z: 25 (20-30)mg/kg/day E: 15 (15-18)mg/kg/day

Other Names:

Ethambutol; isoniazid; rifampicin; pyrazinamide

Outcome Measures

Primary Outcome Measures

number of patients with any grade 3-5 Adverse Event (AE) during treatment, assessed as probably or definitely related to TB treatment [18 months]

Secondary Outcome Measures

number of previously treated patients with H-monoresistance and H-polyresistance, rifampicin (RMP) resistance missed by Xpert Mycobacterium tuberculosis (MTB)/rifampicin (RIF) [18 months]
frequency of initial resistance patterns and mutations conferring resistance
Programmatical effectiveness:number of participants with treatment success divided by number of participants with failure, death, or Lost to follow-up (LTFU) [6 months, 18 months]
6 months treatment success: A patient with smear-positive Pulmonary Tuberculosis (PTB) at the beginning of treatment who completed treatment and sputum smear microscopy (SSM) negative in the last month of treatment and on at least one previous occasion or culture-negative at 6 months. A patient with smear-positive PTB at the beginning of treatment who completed treatment without clinical evidence of failure but with no record of sputum smear or culture results in the last month of treatment (either because tests were not done or because results are unavailable) 18 months treatment success: Those who were cured or completed treatment and were evaluated at 12 months post-treatment to be a) SSM negative , or b) SSM positive but culture (CU) negative, or c) without sputum and no clinical signs of TB.
Clinical effectiveness: number of participants with treatment success, divided by number of participants with failure or death [6 months, 18 months]
6 months treatment success: A patient with smear-positive PTB at the beginning of treatment who completed treatment and SSM negative in the last month of treatment and on at least one previous occasion or culture-negative at 6 months. A patient with smear-positive PTB at the beginning of treatment who completed treatment without clinical evidence of failure but with no record of sputum smear or culture results in the last month of treatment (either because tests were not done or because results are unavailable) 18 months treatment success: Those who were cured or completed treatment and were evaluated at 12 months post-treatment to be a) SSM negative , or b) SSM positive but CU negative, or c) without sputum and no clinical signs of TB.
Bacteriological effectiveness : number of participants with treatment success, divided by number of participants with failure [6 months, 18 months]
6 months treatment success: A patient with smear-positive PTB at the beginning of treatment who completed treatment and SSM negative in the last month of treatment and on at least one previous occasion or culture-negative at 6 months. A patient with smear-positive PTB at the beginning of treatment who completed treatment without clinical evidence of failure but with no record of sputum smear or culture results in the last month of treatment (either because tests were not done or because results are unavailable) 18 months treatment success: Those who were cured or completed treatment and were evaluated at 12 months post-treatment to be a) SSM negative , or b) SSM positive but CU negative, or c) without sputum and no clinical signs of TB.
number of participants with acquired resistance, to Isoniazid (INH) and/or RMP [6 months, 18 months]
In patients with recurrence, the recurrent strain will be compared with the diagnostic strain to identify possible differences in the resistance pattern. If the strain is the same, and resistance is not present in the diagnostic sample but is identified in the recurrence sample, then this resistance is considered as acquired. Resistance is defined as a) on genotypic Drug susceptibility testing (DST) (Deeplex or other): presence of a mutation in the resistance determining region for the drug with exception of generally recognized polymorphisms and silent mutations not leading to an error in the gene product. Heteroresistance at the proportion detectable by these methods will be considered at par with full-blown resistance, or b) growth at the critical concentration for the drug tested in phenotypic DST.
number of participants with stable (without reversion) SSM conversion [2 months]
conversion to 0 AFB per field, without subsequent treatment failure
number of participants with drug-induced hepatotoxicity [18 months]
hepatotoxicity due to anti-TB drug treatment was defined as the following criteria: Grade 3-5 elevation of Liver function test (LFT), or grade 2 elevation of liver function tests with jaundice; AND absence of serological evidence of infection with hepatitis B or C, AND normalization or at least a 50% improvement in abnormal liver chemistry results after withdrawal of anti-TB drugs
number of participants with any TB treatment change due to drug-induced hepatoxicity [18 months]
number of participants with any TB treatment change due to AE [18 months]
number of participants with any grade 3-5 AE [18 months]
number of participants with any Serious Adverse Event (SAE) [18 months]

Eligibility Criteria

Criteria

Ages Eligible for Study:

N/A and Older

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Inclusion Criteria:

All newly registered patients with smear-positive recurrent pulmonary TB
Adults as well as children (no age limit)
Able and willing to provide written informed consent

Exclusion Criteria:

All patients with TB initially resistant to rifampicin on Xpert MTB/RIF testing
Patients transferred to a health facility not supported by the Damien Foundation
Patients previously enrolled in the trial, and with another episode of rifampicin-susceptible TB during the study period
Those with grade III elevation of liver function tests at baseline, or with clinically active liver disease at screening
Pregnant or breastfeeding woman
HIV co-infected patients requiring treatment with a protease inhibitor