Pulmonary Tuberculoses, Other Specified Pulmonary Tuberculosis
Conditions
Keywords
Tuberculosis, Pulmonary, Randomized Controlled Trial (RCT), BTZ-043, Tuberculosis, Antitubercular Agents, Gram-positive Bacterial Infections, Escalating dose, Drug-sensitive TB, Early Bactericidal Activity (EBA), Drug-drug-interaction, Pharmacokinetics (PK), Safety, Tolerability, Bactericidal Activity
Brief summary
This is a prospective, open label, two-centre, randomized, controlled, two-stage, phase Ib/IIa study to evaluate the safety, tolerability, PK, drug-drug interaction and bactericidal activity of BTZ-043 administered orally once daily over 14 days to participants with newly diagnosed, uncomplicated, smear-positive, drug-susceptible pulmonary tuberculosis. The primary objective is to assess the safety and tolerability of BTZ-043 given over 14 days by evaluation of adverse events during treatment and follow-up period in patients with newly diagnosed, uncomplicated, smear-positive, drug-susceptible pulmonary tuberculosis.
Detailed description
This is a prospective, open label, two-centre, randomized, controlled, two-stage, phase Ib/IIa study to evaluate the safety, tolerability, PK, drug-drug interaction and bactericidal activity of BTZ-043 administered orally once daily over 14 days to participants with newly diagnosed, uncomplicated, smear-positive, drug-susceptible pulmonary tuberculosis: Stage 1 is an escalating dose design in up to eight cohorts receiving different doses of BTZ-043 to define a safe dose corridor for BTZ-043. The focus of this stage is on adverse events, PK and a food-effect PK-evaluation . Stage 2 is a parallel group comparison of 4 arms receiving different treatment regimens: three arms to receive BTZ-043 in different doses within the safe corridor defined in stage 1, compared to one arm receiving Rifampicin, Isoniazid, Pyrazinamide, and Ethambutol as a control. This stage is focusing on adverse effects, early bactericidal activity (EBA), PK and an evaluation of PK drug-drug interaction potential. A total of up to 77 male and female patients, aged ≥ 18 - 64 years, with newly diagnosed, smear positive, drug sensitive pulmonary tuberculosis will be enrolled. Allocation of patients will be carried out in two stages: Stage 1: for each cohort 3 patients will be enrolled, treated and followed-up accordingly, starting with cohort 1. In a Trial Steering Committee (TSC) meeting, decision will be made on the dose in the next cohort. Dose escalation steps to be followed, if no safety concerns arise: * Cohort 1: patients to receive 250 mg BTZ-043 * Cohort 2: patients to receive 500 mg BTZ-043 * Cohort 3: patients to receive 750 mg BTZ-043 * Cohort 4: patients to receive 1000 mg BTZ-043 * Cohort 5: patients to receive 1250 mg BTZ-043 * Cohort 6: patients to receive 1500 mg BTZ-043 * Cohort 7: patients to receive 1750 mg BTZ-043 * Cohort 8: patients to receive 2000 mg BTZ-043 Patients receiving the investigational drug in cohorts 1 - 8 will take BTZ-043 in fasting state for 13 days and after a pre-defined high-fat, high-caloric meal on day 14. After all patients of a current cohort have completed at least 7 days of dosing, the TSC, composed of the national principal investigator (PI), the trial statistician, the sponsor representative and two independent scientists, will review safety data, including clinical, lab and electrocardiography (ECG) data, to assess whether dose limiting toxicity of BTZ-043, as defined below, has been observed in any participant. Depending on the outcome, the TSC will then decide on dose escalation, or on enrolling more participants to the same or a lower dose in the following cohort, according to dose escalation and stopping rules. After the end of stage 1, the TSC will decide which of the BTZ-043 doses, which are deemed to not exceed the acceptable toxicity level, are to be moved to stage 2. Stage 2: after the highest possible dose of the investigational drug, that has proven to be safe within the 1st stage, is identified, all remaining patients will be recruited and randomised to receive one of three different doses of BTZ-043 or to control treatment with Rifafour e-275® at a ratio of 3:3:3:2 favouring the experimental treatment. Stage 2 is focusing on adverse effects, early bactericidal activity (EBA), PK and an evaluation of PK drug-drug interaction potential. Allocation of patients: * Arm 1: patients to receive BTZ-043 in a higher dose * Arm 2: patients to receive BTZ-043 in a medium dose * Arm 3: patients to receive BTZ-043 in a lower dose * Control Arm 4: patients to receive Rifafour e-275® as control treatment Participants will take in BTZ-043 in either fasted or fed state, depending on which state has shown to lead to higher exposure during the 1st stage. Additional measurements in the 2nd stage in BTZ-arms 1 to 3 only: • Drug-drug interactions will be investigated: patients, who have been randomized to BTZ-043 arms, will additionally be randomized to receive either a probe drug cocktail, with drugs specifically metabolized by certain enzymes, or dolutegravir at a ratio of 2:1. Probe drugs or Dolutegravir (DTG) will be given pre-BTZ on day 0 and on day 14. After the course of study drugs is completed (on day 14), all patients (in stage 1 and stage 2) will be referred to a government clinic to complete their course of tuberculosis (TB) according to national standards for a total of 6 months of first-line therapy.
Interventions
DRUGBTZ-043
BTZ-043 (250mg per tablet)
DRUGRifafour e-275®
Rifafour e-275® (150mg rifampicin, 75mg isoniazid, 400mg pyrazinamide, 275 mg ethambutol per tablet)
A probe drug cocktail will be given to randomly selected patients after inclusion on Day 1 and on Day 14 once orally. The probe drug cocktail consists of * Caffeine: 1 tablet à 150mg * Tolbutamide: 1/4 tablet à 500mg * Dextromethorphan: 10 ml syrup à 15mg/5ml * Midazolam:2 ml solution à 5mg/5ml * Digoxin: 2 tablets à 0.25mg
1 tablet à 50mg Dolutegravir will be given to randomly selected patients after inclusion on Day 1 and on Day 14 once orally.
Sponsors
European and Developing Countries Clinical Trials Partnership (EDCTP)
Radboud University Medical Center
German Federal Ministry of Education and Research
Michael Hoelscher
Study design
Allocation
RANDOMIZED
Intervention model
SEQUENTIAL
Primary purpose
TREATMENT
Masking
SINGLE (Outcomes Assessor)
Masking description
Laboratory staff, analysing and evaluating the sputum and safety blood samples of the participants will be blinded to the treatment cohort/arm.
Intervention model description
Stage 1: We will enrol patients sequentially in up to 8 cohorts of at least 3 patients to receive BTZ-043 in ascending doses. Patients in the first cohort will receive the lowest dose of 250mg of BTZ-043 for 14 days. After each patient in a cohort has completed at least 7 days, a dosing recommendation for the next cohort will be made using the continual reassessment method (CRM) algorithm. Stage 2: This will be a parallel group comparison of 4 treatment regimens. Patients will be randomized to receive either one of three doses of BTZ-043 within the therapeutic window defined in stage 1, or the control regimen of daily doses of Rifafour e-275®, adapted to body weight, for 14 days in the ratio 3:3:3:2.
Eligibility
Sex/Gender
ALL
Age
18 Years to 64 Years
Healthy volunteers
No
Inclusion criteria
General inclusion criteria: 1. Provide written, informed consent prior to all trial-related procedures including HIV testing. 2. Understand and willing to comply with the study procedures. 3. Male or female adults, aged 18 up to and including 64 years. 4. Body weight ≥ 40 kg. 5. Participants are either unable to conceive/father children AND/OR they will be using two effective methods of contraception, including methods used by the patient's sexual partner(s). At least one to be a barrier method. Disease-specific inclusion criteria: 6. Newly diagnosed, previously untreated, drug-susceptible pulmonary TB 7. Chest X-ray which is consistent with TB 8. Ability to produce an adequate volume of sputum (at least 10ml estimated overnight production) 9. ≥ 1 sputum sample from concentrated sputum positive for acid-fast bacilli on microscopy (at least 1+ on the International Union Against Tuberculosis and Lung Disease/World Health Organization (IUATLD/WHO) scale) from either a spot sputum or overnight sputum sample. General
Exclusion criteria
1. Poor general condition, where delay in treatment cannot be tolerated or death within three months is likely, as assessed by the investigator. 2. The patient is pregnant or breast-feeding. Disease-specific
Design outcomes
Primary
| Measure | Time frame | Description |
|---|---|---|
| Safety and tolerability of BTZ-043 | Day 1 to Day 22 | Safety and tolerability of BTZ-043 will be assessed by evaluation of Adverse Events (AEs) during treatment- and follow-up phase |
Secondary
| Measure | Time frame | Description |
|---|---|---|
| Pharmacokinetic Endpoint - BTZ-043 - Cl | Day 1, 12 and 14 | The PK of BTZ-043 and its two major metabolites BTZ-045S and M2 after a single dose and at steady state will be evaluated by measuring the Clearance (Cl) |
| Bactericidal Activity Endpoint - MGIT | Day -1 to Day 14 | • changes in time to detection in the Mycobacteria Growth Indicator Tube (MGIT™) liquid media culture system from baseline |
| Bactericidal Activity Endpoint - CFU | Day -1 to Day 14 | • changes in solid media colony forming units (CFU) from baseline |
| Bactericidal Activity Endpoint - LAM | Day -1 to Day 14 | • changes in sputum lipoarabinomannan (LAM) concentration from baseline |
| Bactericidal Activity Endpoint - MBLA | Day -1 to Day 14 | • changes in sputum molecular bacterial load assay (MBLA) from baseline |
| Pharmacokinetic Endpoint - BTZ-043 - AUC | Day 1, 12 and 14 | The PK of BTZ-043 and its two major metabolites BTZ-045S and M2 after a single dose and at steady state will be evaluated by measuring the area under the plasma concentration curve (AUC) |
| Pharmacokinetic Endpoint - BTZ-043 - Cmax | Day 1, 12 and 14 | The PK of BTZ-043 and its two major metabolites BTZ-045S and M2 after a single dose and at steady state will be evaluated by measuring the observed maximum concentration (Cmax) |
| Pharmacokinetic Endpoint - BTZ-043 - Tmax | Day 1, 12 and 14 | The PK of BTZ-043 and its two major metabolites BTZ-045S and M2 after a single dose and at steady state will be evaluated by measuring the time to reach Cmax (Tmax) |
| Pharmacokinetic Endpoint - BTZ-043 - Cmin | Day 1, 12 and 14 | The PK of BTZ-043 and its two major metabolites BTZ-045S and M2 after a single dose and at steady state will be evaluated by measuring the minimum observed plasma concentration 24 hours following the last dose (Cmin) |
| Pharmacokinetic Endpoint - BTZ-043 - Vd | Day 1, 12 and 14 | The PK of BTZ-043 and its two major metabolites BTZ-045S and M2 after a single dose and at steady state will be evaluated by measuring the Volume of distribution (Vd) |
| Pharmacokinetic Endpoint - BTZ-043 - T1/2 | Day 1, 12 and 14 | The PK of BTZ-043 and its two major metabolites BTZ-045S and M2 after a single dose and at steady state will be evaluated by measuring the Elimination half-life (T1/2) |
| Pharmacokinetic Endpoint - BTZ-043 - pharmacodynamics (PD) | Day 1, 12 and 14 | The PK of BTZ-043 and its two major metabolites BTZ-045S and M2 after a single dose and at steady state will be evaluated by measuring the Relation of efficacy measurements to pharmacokinetic indices of BTZ-043 and its metabolites (AUC, Cmax) |
| Pharmacokinetic Endpoint - Population PK AUC | Day 1, 12 and 14 | A population PK-analysis of BTZ-043 and its two major metabolites will be carried out by measuring the AUC and describing PK differences of BTZ-043 and its main metabolites between subjects to quantify inter-individual variability, suitable for evaluation of alternative dosing regimens |
| Pharmacokinetic Endpoint - Population PK Cmax | Day 1, 12 and 14 | A population PK-analysis of BTZ-043 and its two major metabolites will be carried out by measuring the Cmax and describing PK differences of BTZ-043 and its main metabolites between subjects to quantify inter-individual variability, suitable for evaluation of alternative dosing regimens |
| Pharmacokinetic Endpoint - Food Effect PK AUC | Day 14 | The effect of food on the exposure of the BTZ-043 and its two major metabolites will be determined by measuring the AUC of BTZ-043 and its main metabolites and by evaluating the change after a high fat high calorie meal in comparison to the AUC under fasting conditions during the 1st stage. |
| Pharmacokinetic Endpoint - Food Effect PK Cmax | Day 14 | The effect of food on the exposure of the BTZ-043 and its two major metabolites will be determined by measuring the Cmax of BTZ-043 and its main metabolites and by evaluating the change after a high fat high calorie meal in comparison to the Cmax under fasting conditions during the 1st stage. |
| Pharmacokinetic Endpoint - Probe Drugs PK AUC | Day 0 and 14 | The effect on BTZ-043 at steady state on hepatic enzyme and P-glycoprotein activity (induction vs. inhibition) will be evaluated by measuring changes in AUC of the probe drugs administered on day 0, and day 14 during the 2nd stage. |
| Pharmacokinetic Endpoint - Probe Drugs PK Cmax | Day 0 and 14 | The effect on BTZ-043 at steady state on hepatic enzyme and P-glycoprotein activity (induction vs. inhibition) will be evaluated by measuring changes in Cmax of the probe drugs administered on day 0, and day 14 during the 2nd stage. |
Countries
South Africa
Outcome results
None listed