Triage Test for All Oral DR-TB Regimen (TRiAD Study)

Recruiting

• Conditions: Drug Resistant Tuberculosis; Tuberculosis; MDR-TB; XDR-TB
• Interventions: Diagnostic Test: Xpert® MTB/XDR

• Registration Number: NCT05175794
• Lead Sponsor: Centre for the AIDS Programme of Research in South Africa

Brief Summary

A Phase 4 operational study to assess the effectiveness, feasibility, acceptability, and cost effectiveness of the GeneXpert MTB/XDR (Xpert XDR; Cepheid) assay for rapid triage-and-treatment of DR-TB-A multi-centre, multi-country prospective cohort study

Detailed Description

The TriAD study is a multi-center, multi-country Prospective Pragmatic Cohort study assessing the effectiveness, feasibility, acceptability, and cost-effectiveness of implementing the Xpert MTB/XDR (Xpert XDR; Cepheid) assay for rapid triage-and-treatment with short, all- oral drug resistant tuberculosis (DR-TB) treatment. The proposed study aims to screen approximately 4800 GeneXpert MTB/RIF or Ultra MTB-positive (irrespective of rifampicin resistance status) patients from 9 study sites in South Africa, Nigeria and Ethiopia to enrol 880 rifampicin resistant (RR) and 400 isoniazid mono-resistant (HR) patients over a period of 12-18 months. The Xpert XDR assay, a rapid genotypic test, will be implemented as a reflex test to detect resistance to isoniazid, fluoroquinolones and second-line injectable agents to provide rapid genotypic susceptibility testing for DR-TB detection. Patients that test positive for Mycobacterium tuberculosis with rifampicin resistance will be enrolled in Cohort 1 (n=880). Patients that test positive for Mycobacterium tuberculosis that are rifampicin susceptible with isoniazid mono-resistance will be enrolled in Cohort 2 (n=400). Results from the Xpert XDR assay will be used to guide selection of appropriate, evidence-based, all-oral DR-TB treatment regimens of shortest possible duration. The tuberculosis molecular bacterial load assay (TB-MBLA) will be used as an adjunct to provide bacillary load monitoring over the course of treatment to assess real-time treatment response. Operational research will provide information about the feasibility, acceptability and cost-effectiveness to inform policies and guidelines for programmatic implementation of the triage-and-treat model.

Study Timeline

• Study First Submitted: 2021-09-22
• Study First Submitted QC: 2021-12-14
• Study First Posted: 2022-01-04
• Study Start: 2022-05-26
• Status Verified: 2024-02
• Last Update Submitted: 2024-02-16
• Last Update Posted: 2024-02-20
• Primary Completion: 2024-12-31
• Study Completion: 2025-06-01

Recruitment & Eligibility

• Status: RECRUITING
• Sex: All
• Target Recruitment: 1280

Inclusion Criteria

1. Ambulant adults ≥ 18 years of age

2. Newly diagnosed PTB patients receiving less than 5 days of treatment since new diagnosis:

   1. Cohort 1: < 5 days of DR-TB treatment
   2. Cohort 2: < 5 days of INH mono-resistant TB treatment preceding study entry for the current TB episode, or

3. Sputum positive (smear and or culture) TB patients classified as failing first line treatment

4. Any currently available Nucleic Acid Amplification Tests for drug-resistance detection changes/assay positive for M.tb infection with:

   Cohort 1: at least Rifampicin resistance Cohort 2: Rifampicin susceptible co-occurring with INH, fluoroquinolone, ethionamide or aminoglycoside resistance (detected by Xpert XDR) occurring alone or in combination

5. Capacity to provide informed consent

6. HIV infected and uninfected participants are allowed in the study. Participants already on ART will be allowed in the study provided the ART regimen in use has no contraindications to the proposed TB drug regimen

7. Willing to have samples collected, stored indefinitely, and used for research purposes

8. Able to provide reasonable proof of identity (to satisfaction of study team member) at or prior to enrolment

Exclusion criteria:

1. Has a known severe allergy to any of the BPaL component drugs
2. Has DST showing infection with a strain resistant to any of the component drugs
3. Has TB meningitis, other central nervous system TB, or TB osteomyelitis; or
4. Is pregnant or breastfeeding
5. Is unable to take oral medications
6. Persons with any other medical condition, precluding study participation based on investigator judgement
7. Any co-existing condition that in the opinion of the attending clinician renders the participant unsuitable for participation in the study
8. Co-enrolment in other interventional research studies

Exclusion Criteria

Not provided

Study & Design

• Study Type: OBSERVATIONAL
• Study Design: Not specified

Arm && Interventions

Group	Intervention	Description
Cohort 1	Xpert® MTB/XDR	Participants that test positive for Mycobacterium tuberculosis (M.tb) with rifampicin resistance will be enrolled in Cohort 1 (n=880).
Cohort 2	Xpert® MTB/XDR	Participants that test positive for M.tb that are rifampicin susceptible with isoniazid mono-resistance will be enrolled in Cohort 2 (n=400).

Primary Outcome Measures

Name	Time	Method
Time to initiation	4 years	Time to initiation of an appropriate all oral treatment regimen from date of first sputum collected
Proportion of patients with favorable treatment outcomes	4 years	Proportion of patients with favorable treatment outcomes at month 12 from diagnosis

Secondary Outcome Measures

Name	Time	Method
Time to culture Conversion	4 years	Time specific rates of culture conversion
HR TB Prevalence	4 years	Prevalence of HR TB (cohort 2)
Adverse Drug Reactions	4 years	Incidence of adverse drug reactions documented during all oral treatment
Mortality	4 years	All cause mortality documented during treatment and follow up
XDR TB Prevalence	4 years	Prevalence of XDR TB (cohort 2)
Quality of Xpert XDR testing	4 years	Quality of Xpert XDR testing will be assessed using: 1. indeterminate rates measured by the number of Xpert XDR tests regarded as invalid divided by the total number of Xpert XDR tests performed; 2. Contamination rates or frequency of DNA contamination: number of Xpert XDR tests flagging contamination divided by the total number of Xpert XDR tests performed or events; 3. performance variation will be measured by performance in discrimination of (i) INH resistance compared to culture across study sites, (ii) aminoglycoside resistance compared to culture across study sites and (iii) fluroquinolone resistance compared to culture across study sites
Cost effectiveness	4 years	Data for Costing studies will be collected through semi-structured interviews of key informants and document review. Methods will include a construction of incremental cost effectiveness ratios (ICER) and CE-model to estimate the costs and benefits from a societal perspective, generalizable to other settings.; timely initiated on treatment
Operational Feasibility of patient triaging	4 years	The Operational Cost including Infrastructure and Human resource requirements for the study approach.
Proportion of patients with Bedaquiline and linezolid resistance not eligible for short course treatment	4 years	Proportion of patients with Bedaquiline and linezolid resistance not eligible for short course treatment
Clinical utility of the Tuberculosis Molecular Bacterial Load Assay (TB-MBLA) compared to routine culture to monitor DR-TB treatment response	4 years	Quantitative results from the TB-MBLA, a real-time quantitative PCR (RT-qPCR) assay, that detects and quantifies killing of 16S rRNA from both viable replicating and dormant M. tuberculosis in patient sputum during treatment, will be compared to routine culture in monitoring treatment response
Feasibility of Tuberculosis Molecular Bacterial Load Assay (TB-MBLA) will be compared to routine culture in bacteriological follow-up for people on DR-TB treatment	4 years	Feasibility of TB-MBLA Assessed by comparison to liquid culture with respect to accuracy, result turn-around time, failure rates.
Accuracy of Xpert XDR testing compared to WGS	4 years	The performance of Xpert XDR will be compared to Culture DST, LPA and Next Generation Sequencing.
Resistance profile of sputum samples for identification of drug resistance mutations as per pre-existing probes within the Xpert XDR assay	4 years	Cultured isolates from the same sputum sample will undergo WGS sequencing to identify additional resistance mutations to new and re-purposed drugs. The endpoints measured for this objective includes: 1. Frequency of detection of additional resistance conferring mutations by WGS not detected by Xpert XDR; 2. Impact of these previously undetected mutation on conferring resistance to the new drugs in the bedaquiline, pretomanid and linezolid regimen

Trial Locations

Locations (4)

CAPRISA Springfield Research Clinic; 🇿🇦 Durban, KwaZulu-Natal, South Africa

Ethiopian Public Health Institute (EPHI); 🇪🇹 Gulele, Addis Ababa, Ethiopia

Institute of Human Virology Nigeria; 🇳🇬 Yaba, Lagos State, Nigeria

Clinical HIV Research Unit (CHRU), WITS Health Consortium; 🇿🇦 Bethelsdorp, Port Elizabeth, South Africa