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Evaluating the Safety, Tolerability, and Pharmacokinetics of Bedaquiline and Delamanid, Alone and in Combination, For Drug-Resistant Pulmonary Tuberculosis

A Trial of the Safety, Tolerability, and Pharmacokinetics of Bedaquiline and Delamanid, Alone and in Combination, Among Participants Taking Multidrug Treatment for Drug-Resistant Pulmonary Tuberculosis

Status
Completed
Phases
Phase 2
Study type
Interventional
Source
ClinicalTrials.gov
Registry ID
NCT02583048
Enrollment
84
Registered
2015-10-21
Start date
2016-08-15
Completion date
2021-02-04
Last updated
2022-01-27

For informational purposes only — not medical advice. Sourced from public registries and may not reflect the latest updates. Terms

Conditions

Tuberculosis, HIV Infections

Brief summary

This study evaluated the safety, tolerability, and pharmacokinetics of the anti-tuberculosis (TB) drugs bedaquiline (BDQ) and delamanid (DLM), alone and in combination, among participants (with or without HIV co-infection) taking multidrug treatment for multidrug-resistant tuberculosis (MDR-TB) or rifampin-monoresistant TB (RR-TB).

Detailed description

Bedaquiline (BDQ) and delamanid (DLM) are two newly approved anti-TB drugs and are both well tolerated. However, the combined effect of these two drugs has not been studied. Combining these two drugs, together with other anti-TB drugs, may improve outcomes for people with MDR-TB or RR-TB. The purpose of this study was to evaluate the safety, tolerability, and pharmacokinetics of BDQ and DLM, alone and in combination, among participants (with or without HIV co-infection) taking multidrug treatment for MDR-TB or RR-TB, and specifically to evaluate the effect of these drugs on the heart. Participants were randomly assigned to one of three arms: participants in Arm 1 received BDQ, participants in Arm 2 received DLM, and participants in Arm 3 received BDQ and DLM. All participants received their assigned study drugs for 24 weeks together with multidrug background treatment (MBT) for MDR-TB or RR-TB (not provided by the study). HIV-infected participants also received dolutegravir, to be used in combination with two nucleoside reverse transcriptase inhibitors (NRTIs) until study completion. NRTIs were not provided by the study. At study entry participants were initially required to be hospitalized for 2 months, however after an interim analysis, the period of hospitalization was shortened to 2 weeks. Study visits occurred at entry, each week for 8 weeks after study entry, every other week until week 24, and at weeks 28, 36, 48, 60, 72, 84, 96 and 128. Visits included physical examinations, blood collection, urine collection, sputum sample collection, hair sample collection, chest x-rays, pregnancy testing, electrocardiograms (ECGs), and adherence questionnaires. Participants were also asked to take part in an optional cerebrospinal fluid sampling study that entailed a lumbar puncture, to be done at weeks 8 or 24.

Interventions

DRUGBedaquiline

Four 100 mg tablets (400 mg) orally once a day for 2 weeks, followed by two 100 mg tablets (200 mg) orally three times a week for 22 weeks.

DRUGDelamanid

Two 50 mg tablets (100 mg) orally with food twice a day for 24 weeks.

DRUGDolutegravir

For HIV-positive participants only: one 50 mg tablet orally once daily, to be used in combination with two NRTIs until study completion. (NRTIs were not provided by the study.)

DRUGMultidrug Background Treatment (MBT) for TB

A standardized MBT regimen for MDR- or RR-TB except in cases where a participant had known resistance to one of the components of local standard treatment. MBT was provided by the local program.

Sponsors

National Institute of Allergy and Infectious Diseases (NIAID)
Lead SponsorNIH

Study design

Allocation
RANDOMIZED
Intervention model
PARALLEL
Primary purpose
TREATMENT
Masking
NONE

Eligibility

Sex/Gender
ALL
Age
18 Years to No maximum
Healthy volunteers
No

Inclusion criteria

* Documented pulmonary infection due to strains of MTB with (a) resistance to isoniazid (INH) and rifampin (RIF) (MDR-TB) or (b) resistance to RIF but not INH (RR-TB) from a sputum sample collected within 60 days prior to entry. * Laboratory confirmation of infection with an MTB strain that is susceptible to fluoroquinolones and aminoglycosides within 60 days prior to entry. * HIV-1 infection status documented as either absent or present, as defined below: * Absence of HIV-1 infection, within 60 days prior to entry. OR * HIV-1 infection * For HIV-positive participants only: CD4+ count greater than or equal to 100 cells/mm\^3 within 60 days prior to entry. * For HIV-positive participants only: For participants on ART for greater than or equal to 6 months and have an HIV-1 viral load greater than 500 copies/mL within 60 days prior to entry, a HIV-1 genotype within 60 days prior to entry must have shown that at least one fully active NRTI was available to the participant within the country program. * For females of reproductive potential, a negative serum pregnancy test within 48 hours prior to entry * All participants of reproductive potential who are participating in sexual activity that could lead to pregnancy must have agreed to use one method of birth control while receiving TB study medications and for 6 months after stopping TB study medications. * Participants who were not of reproductive potential were eligible without requiring the use of contraceptives. * For HIV-positive female participants of reproductive potential, the use of contraceptives was required for the full duration of time the participant was taking dolutegravir (ie, through study completion at week 128). * Chest x-ray performed within 60 days prior to entry to classify participant as having cavitary or non-cavitary disease * Documentation of Karnofsky performance score greater than or equal to 50 within 14 days prior to study entry * Ability and willingness of participant or legally authorized representative to provide informed consent * Willingness to be hospitalized for the required inpatient component of the study * Taking MBT for a minimum of 7 days within the 10 days prior to entry

Exclusion criteria

* History of clinically relevant, currently active or underlying gastrointestinal, hepatic, cardiovascular, nervous system, psychiatric, metabolic (e.g., untreated hypothyroidism), renal, respiratory (other than due to TB), inflammatory, neoplastic, skin, immunological or infectious disease, which is not stable and controlled, that in the opinion of the investigator would preclude safe participation in the trial * Current clinically relevant extrapulmonary TB, in the opinion of the site investigator, including but not limited to central nervous system (CNS) TB or TB osteoarthritis * Previous treatment for MDR- or RR-TB, other than for the qualifying episode, at any time in the past * Receipt of BDQ or DLM at any time in the past * Breastfeeding * QTcF interval greater than 450 ms within 72 hours prior to entry * Clinically significant ECG abnormality in the opinion of the site investigator within 60 days prior to entry, including but not limited to second or third degree atrioventricular (AV) block, prolongation of the QRS complex over 120 ms (in both male and female participants), or clinically important arrhythmia * Current clinically relevant cardiovascular disorder in the opinion of the site investigator, including but not limited to heart failure, coronary heart disease, arrhythmia, or tachyarrhythmia * Known family history of Long QT Syndrome in a first-degree relative (i.e., parent, offspring, or sibling) * Requirement or expected requirement for protease inhibitors (PIs), efavirenz (EFV), or any other medication that is a moderate to strong inhibitor or inducer of CYP3A and CYP3A4 over the 24 weeks of study treatment. NOTE: Participants taking a PI or EFV can be switched to a treatment that is allowed in the study, but the PI must be stopped at least 2 days prior to starting study MDR- or RR-TB drugs and EFV must be stopped at least 7 days prior to starting study MDR- or RR-TB drugs. * Requirement or expected requirement for a medication that significantly prolongs QTc, including but not limited to moxifloxacin (levofloxacin is acceptable), from 72 hours prior to study entry through 4 weeks after discontinuation of study treatment (week 28) * Requirement or expected requirement of clofazimine, from 7 days prior to study entry through week 24 (discontinuation of study treatment). * For individuals receiving the WHO short course regimen that contains clofazimine, receipt of more than 21 cumulative days of clofazimine at any time prior to, or at the time of, study entry. * Known allergy/sensitivity or any hypersensitivity to components of study TB drugs or their formulation or to the nitroimidazole class of antibiotics * Active drug or alcohol use or dependence that, in the opinion of the site investigator, would interfere with adherence to study requirements * Any of the following laboratory abnormalities within 14 days prior to entry: 1. Serum creatinine greater than 1.4 x upper limit of normal (ULN) 2. Lipase greater than 1.6 x ULN 3. Alanine aminotransferase (ALT) greater than 2.5 x ULN 4. Total bilirubin greater than 1.6 x ULN 5. Potassium less than 3.4 or greater than 5.6 mmol/L; magnesium less than 0.59 mmol/L; calcium less than 1.75 mmol/L * Known current hepatitis B or C infection, current treatment for hepatitis B or hepatitis C infection, or positive for hepatitis B surface antigen or hepatitis C antibodies within 60 days prior to entry * Among participants with HIV infection, in whom use of dolutegravir (DTG) is anticipated, any of the following: 1. Unstable liver disease (as defined by the presence of ascites, encephalopathy, coagulopathy, esophageal varices, or persistent jaundice), known biliary abnormalities (with the exception of Gilbert's syndrome or asymptomatic gallstones) 2. History or presence of allergy to DTG or its components 3. Severe hepatic impairment (Class C) as determined by Child-Pugh classification 4. Previous use of raltegravir * Documentation of any new and/or unstable AIDS-defining illness (other than TB) as defined by the CDC within 60 days prior to entry * Acute or serious illness (other than TB) requiring systemic treatment and/or hospitalization within 60 days prior to entry

Design outcomes

Primary

MeasureTime frameDescription
Mean Change From Baseline in QTcFBaseline and at weeks 8, 10, 12, 14, 16, 18, 20, 22 and 24Mean change from baseline in QTcF (ie, QTcF prolongation) in milliseconds (ms), where baseline QTcF was represented by QTcF durations measured at week 0, and post-baseline QTcF was represented by QTcF durations measured at weeks 8 through 24 (pooled). QTcF calculated as average of 1-3 available QTcF values per visit.
Post-Baseline QTcFBaseline and at weeks 8, 10, 12, 14, 16, 18, 20, 22, and 24.Baseline and post-baseline absolute QTcF in milliseconds (ms) estimated using an ANOVA model, where baseline QTcF was represented by QTcF durations measured at week 0, and post-baseline QTcF was represented by QTcF durations measured at weeks 8 through 24 (pooled). QTcF calculated as average of 1-3 available QTcF values per visit. Interim analysis conducted when week 24 QT data was available for ≥12 participants stipulated 99.9% confidence interval; original coverage of 95% was widened to 95.1%.

Secondary

MeasureTime frameDescription
Changes in QTcF From BaselineBaseline and at weeks 2, 4, 6, 8, 10, 12, 14, 16, 18, 20, 22, 24 and 28.Change from baseline in QTcF, calculated as the difference between each post-baseline week and week 0. (QTcF calculated as average of 1-3 available QTcF values per visit.)
Percentage of Participants With an Occurrence of QTcF >480 and ≤500 Milliseconds (ms)At weeks 2, 4, 6, 8, 10, 12, 14, 16, 18, 20, 22 and 24Participants who experienced QTcF \>480 and ≤500 ms at least once at any time from week 2 to 24. QTcF calculated as average of 1-3 available QTcF values per visit.
Percentage of Participants With an Occurrence of QTcF Increase From Baseline of >30 and ≤60 Milliseconds (ms)Baseline and at weeks 2, 4, 6, 8, 10, 12, 14, 16, 18, 20, 22 and 24Participants who experienced QTcF increase from baseline of \>30 and ≤60 ms at least once at any time from week 2 to 24. QTcF calculated as average of 1-3 available QTcF values per visit.
BDQ PK Parameter Minimum Plasma Concentration (Cmin) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Intensive BDQ PK samples at pre-dose, 5h, 7h, 10h and 22h post-dose at weeks 2, 8 and 24This evaluates the effect of DLM on the BDQ PK parameter Cmin obtained from participants enrolled in Arms 1 and 3 (without and with co-administration of DLM). Cmin defines minimum concentration observed over the first 22 hours of the BDQ dosing interval.
BDQ PK Parameter Maxmum Plasma Concentration (Cmax) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Intensive BDQ PK samples at pre-dose, 5h, 7h, 10h and 22h post-dose at weeks 2, 8 and 24This evaluates the effect of DLM on the BDQ PK parameter Cmax obtained from participants enrolled in Arms 1 and 3 (without and with co-administration of DLM). Cmax defines maximum concentration observed over the first 22 hours of the BDQ dosing interval.
BDQ PK Parameter Area Under the Concentration Time Curve (AUC 0-22h) Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Intensive BDQ PK samples at pre-dose, 5h, 7h, 10h and 22h post-dose at Weeks 2, 8 and 24This evaluates the effect of DLM on the BDQ PK parameter AUC 0-22h obtained from participants enrolled in Arms 1 and 3 (without and with co-administration of DLM). AUC 0-22h defines area under the concentration-time curve over the period of 22 hours post-dose.
N-monodesmethyl Metabolite of BDQ PK Parameter Cmin Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Intensive BDQ Metabolite PK samples at pre-dose, 5h, 7h, 10h and 22h post-dose at weeks 2, 8 and 24This evaluates the effect of DLM on the N-monodesmethyl Metabolite of BDQ PK parameter Cmin obtained from participants enrolled in Arms 1 and 3 (without and with co-administration of DLM). Cmin defines minimum concentration observed over the first 22 hours of the BDQ dosing interval.
N-monodesmethyl Metabolite of BDQ PK Parameter Cmax Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Intensive BDQ Metabolite PK samples at pre-dose, 5h, 7h, 10h and 22h post-dose at weeks 2, 8 and 24This evaluates the effect of DLM on the BDQ Metabolite N-monodesmethyl BDQ PK parameter Cmax obtained from participants enrolled in Arms 1 and 3 (without and with co-administration of DLM). Cmax defines maximum concentration observed over the first 22 hours of the BDQ dosing interval.
N-monodesmethyl Metabolite of BDQ PK Parameter AUC 0-22h Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Intensive BDQ PK samples at pre-dose, 5h, 7h, 10h and 22h post-dose at Weeks 2, 8 and 24This evaluates the effect of DLM on the N-monodesmethyl Metabolite of BDQ PK parameter AUC 0-22h obtained from participants enrolled in Arms 1 and 3 (without and with co-administration of DLM). AUC 0-22h defines area under the concentration-time curve over the period of 22 hours post-dose.
Percentage of Participants With an Occurrence of QTcF Greater Than 500 Milliseconds (ms)At weeks 2, 4, 6, 8, 10, 12, 14, 16, 18, 20, 22 and 24Participants who experienced QTcF greater than 500 ms at least once at any time from week 2 to 24. QTcF calculated as average of 1-3 available QTcF values per visit.
DLM PK Parameter Cmax Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Intensive DLM PK samples at pre-dose, 4h, 8h, and 11h post-dose at weeks 2, 8 and 24This evaluates the effect of BDQ on the DLM PK parameter Cmax obtained from participants enrolled in Arms 2 and 3 (without and with co-administration of BDQ). Cmax defines maximum concentration observed over the first 11 hours of the DLM dosing interval.
DLM PK Area Under the Concentration Time Curve (AUC 0-11h) Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Intensive DLM PK samples at pre-dose, 4h, 8h, and 11h post-dose at weeks 2, 8 and 24This evaluates the effect of BDQ on the DLM PK parameter AUC 0-11h obtained from participants enrolled in Arms 2 and 3 (without and with co-administration of BDQ). AUC 0-11h defines area under the concentration-time curve over the first 11 hours of the DLM dosing interval.
DLM Metabolite DM6705 PK Parameter Cmin Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Intensive DLM PK samples at pre-dose, 4h, 8h, and 11h post-dose at weeks 2, 8 and 24This evaluates the effect of BDQ on the DLM Metabolite DM6705 PK parameter Cmin obtained from participants enrolled in Arms 2 and 3 (without and with co-administration of BDQ). Cmin defines minimum concentration observed over the first 11 hours of the DLM dosing interval.
DLM Metabolite DM6705 PK Parameter Cmax Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Intensive DLM PK samples at pre-dose, 4h, 8h, and 11h post-dose at weeks 2, 8 and 24This evaluates the effect of BDQ on the DLM Metabolite DM6705 PK parameter Cmax obtained from participants enrolled in Arms 2 and 3 (without and with co-administration of BDQ). Cmax defines maximum concentration observed over the first 11 hours of the DLM dosing interval.
DLM Metabolite DM6705 PK AUC 0-11h Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Intensive DLM PK samples at pre-dose, 4h, 8h, and 11h post-dose at weeks 2, 8 and 24This evaluates the effect of BDQ on the DLM Metabolite DM6705 PK parameter AUC 0-11h obtained from participants enrolled in Arms 2 and 3 (without and with co-administration of BDQ). AUC 0-11h defines area under the concentration-time curve over the first 11 hours of the DLM dosing interval.
Percentage of Participants With an Occurrence of Grade 3 or Higher Adverse EventFrom initiation of study TB treatment (week 0) to week 24Participants with an occurrence of an adverse event (laboratory value, sign/symptom, diagnosis) of grade 3 or 4. Severity grading based on DAIDS AE Grading Table Version 2.0. Participants were counted once at the highest grade (grade 3 or grade 4).
Percentage of Participants Who Discontinued Study TB Drug(s) For Any ReasonFrom initiation of study TB treatment (week 0) to week 24Percentage of participants who discontinued study TB drug(s) for any reason
Percentage of Participants Who DiedFrom initiation of study TB treatment (week 0) to week 24Among participants who took at least one dose of study TB treatment, percentage of participants who died on or before week 24. Note that the all-cause mortality includes deaths that occurred at any time during treatment or follow-up through week 128.
DLM PK Parameter Cmin Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Intensive DLM PK samples at pre-dose, 4h, 8h, and 11h post-dose at weeks 2, 8 and 24This evaluates the effect of BDQ on the DLM PK parameter Cmin obtained from participants enrolled in Arms 2 and 3 (without and with co-administration of BDQ). Cmin defines minimum concentration observed over the first 11 hours of the DLM dosing interval.
Percentage of Participants With an Increase in QTcF From Baseline of Greater Than 60 Milliseconds (ms)Baseline and at weeks 2, 4, 6, 8, 10, 12, 14, 16, 18, 20, 22 and 24Participants who experienced QTcF increase from baseline greater than 60 ms at least once at any time from week 2 to 24. QTcF calculated as average of 1-3 available QTcF values per visit.

Countries

Peru, South Africa

Participant flow

Recruitment details

Participants were enrolled from August 2016 to July 2018 at 3 non-US clinical research sites.

Pre-assignment details

Participants were randomized with equal probability to each of the 3 experimental arms.

Participants by arm

ArmCount
Arm 1: Bedaquiline
Participants received 400 mg of bedaquiline once a day for 2 weeks followed by 200 mg of bedaquiline three times a week for 22 weeks. For HIV-positive participants only: One 50 mg tablet of Dolutegravir was taken orally once daily, to be used in combination with two NRTIs until study completion. (NRTIs not provided by the study.) Participants also took Multidrug Background Treatment (MBT) for TB (not provided by the study).
28
Arm 2: Delamanid
Participants received 100 mg of delamanid twice a day for 24 weeks. For HIV-positive participants only: One 50 mg tablet of Dolutegravir was taken orally once daily, to be used in combination with two NRTIs until study completion. (NRTIs not provided by the study.) Participants also took Multidrug Background Treatment (MBT) for TB (not provided by the study).
28
Arm 3: Bedaquiline and Delamanid
Participants received 400 mg of bedaquiline once a day and 100 mg of delamanid twice a day for 2 weeks. They then received 200 mg of bedaquiline three times a week and 100 mg of delamanid twice a day for 22 weeks. For HIV-positive participants only: One 50 mg tablet of Dolutegravir was taken orally once daily, to be used in combination with two NRTIs until study completion. (NRTIs not provided by the study.) Participants also took Multidrug Background Treatment (MBT) for TB (not provided by the study).
28
Total84

Withdrawals & dropouts

PeriodReasonFG000FG001FG002
Overall StudyFailed to meet eligibility criterion001
Overall StudyWithdrawal by Subject010

Baseline characteristics

CharacteristicArm 1: BedaquilineArm 2: DelamanidArm 3: Bedaquiline and DelamanidTotal
Age, Continuous34.5 years32 years34 years34 years
Baseline QTcF394.3 milliseconds406.2 milliseconds387.3 milliseconds395.5 milliseconds
HIV-1 Positive10 Participants11 Participants10 Participants31 Participants
Race/Ethnicity, Customized
Black African
16 Participants11 Participants11 Participants38 Participants
Race/Ethnicity, Customized
Coloured
11 Participants13 Participants14 Participants38 Participants
Race/Ethnicity, Customized
Mestizo
1 Participants2 Participants3 Participants6 Participants
Race/Ethnicity, Customized
Other
0 Participants1 Participants0 Participants1 Participants
Race/Ethnicity, Customized
White
0 Participants1 Participants0 Participants1 Participants
Region of Enrollment
Peru
1 Participants2 Participants3 Participants6 Participants
Region of Enrollment
South Africa
27 Participants26 Participants25 Participants78 Participants
Sex: Female, Male
Female
6 Participants7 Participants8 Participants21 Participants
Sex: Female, Male
Male
22 Participants21 Participants20 Participants63 Participants

Adverse events

Event typeEG000
affected / at risk
EG001
affected / at risk
EG002
affected / at risk
deaths
Total, all-cause mortality
0 / 281 / 270 / 27
other
Total, other adverse events
21 / 2816 / 2721 / 27
serious
Total, serious adverse events
2 / 283 / 278 / 27

Outcome results

Primary

Mean Change From Baseline in QTcF

Mean change from baseline in QTcF (ie, QTcF prolongation) in milliseconds (ms), where baseline QTcF was represented by QTcF durations measured at week 0, and post-baseline QTcF was represented by QTcF durations measured at weeks 8 through 24 (pooled). QTcF calculated as average of 1-3 available QTcF values per visit.

Time frame: Baseline and at weeks 8, 10, 12, 14, 16, 18, 20, 22 and 24

Population: Participants with a baseline QTcF measurement, and at least one post-baseline QTcF measurement from a visit conducted at week 8 through 24, prior to permanent discontinuation of study Tuberculosis (TB) drug and without a temporary discontinuation of study TB drug of 7 or more days immediately preceding the measurement.

ArmMeasureValue (MEAN)
Arm 1: BedaquilineMean Change From Baseline in QTcF12.3 milliseconds (ms)
Arm 2: DelamanidMean Change From Baseline in QTcF8.6 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidMean Change From Baseline in QTcF20.7 milliseconds (ms)
95.1% CI: [2, 14.8]
95.1% CI: [5.7, 18.6]
Primary

Post-Baseline QTcF

Baseline and post-baseline absolute QTcF in milliseconds (ms) estimated using an ANOVA model, where baseline QTcF was represented by QTcF durations measured at week 0, and post-baseline QTcF was represented by QTcF durations measured at weeks 8 through 24 (pooled). QTcF calculated as average of 1-3 available QTcF values per visit. Interim analysis conducted when week 24 QT data was available for ≥12 participants stipulated 99.9% confidence interval; original coverage of 95% was widened to 95.1%.

Time frame: Baseline and at weeks 8, 10, 12, 14, 16, 18, 20, 22, and 24.

Population: Participants with a baseline QTcF measurement, and at least one post-baseline QTcF measurement from a visit conducted at week 8 through 24, prior to permanent discontinuation of study Tuberculosis (TB) drug and without a temporary discontinuation of study TB drug of 7 or more days immediately preceding the measurement.

ArmMeasureGroupValue (LEAST_SQUARES_MEAN)
Arm 1: BedaquilinePost-Baseline QTcFBaseline397.4 milliseconds (ms)
Arm 1: BedaquilinePost-Baseline QTcFPost-baseline409.7 milliseconds (ms)
Arm 2: DelamanidPost-Baseline QTcFBaseline404.9 milliseconds (ms)
Arm 2: DelamanidPost-Baseline QTcFPost-baseline413.4 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidPost-Baseline QTcFBaseline391.7 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidPost-Baseline QTcFPost-baseline412.4 milliseconds (ms)
Secondary

BDQ PK Parameter Area Under the Concentration Time Curve (AUC 0-22h) Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3

This evaluates the effect of DLM on the BDQ PK parameter AUC 0-22h obtained from participants enrolled in Arms 1 and 3 (without and with co-administration of DLM). AUC 0-22h defines area under the concentration-time curve over the period of 22 hours post-dose.

Time frame: Intensive BDQ PK samples at pre-dose, 5h, 7h, 10h and 22h post-dose at Weeks 2, 8 and 24

Population: Participants who took at least one dose of study treatment, and were taking study drug at the time of the PK visit.

ArmMeasureGroupValue (MEAN)Dispersion
Arm 1: BedaquilineBDQ PK Parameter Area Under the Concentration Time Curve (AUC 0-22h) Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Week 231570.9 ng*h/mLStandard Deviation 14612.8
Arm 1: BedaquilineBDQ PK Parameter Area Under the Concentration Time Curve (AUC 0-22h) Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Week 819234.6 ng*h/mLStandard Deviation 7785.7
Arm 1: BedaquilineBDQ PK Parameter Area Under the Concentration Time Curve (AUC 0-22h) Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Week 2421048.5 ng*h/mLStandard Deviation 8329.7
Arm 2: DelamanidBDQ PK Parameter Area Under the Concentration Time Curve (AUC 0-22h) Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Week 232399.4 ng*h/mLStandard Deviation 13625.2
Arm 2: DelamanidBDQ PK Parameter Area Under the Concentration Time Curve (AUC 0-22h) Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Week 820176.1 ng*h/mLStandard Deviation 8175.5
Arm 2: DelamanidBDQ PK Parameter Area Under the Concentration Time Curve (AUC 0-22h) Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Week 2419522.6 ng*h/mLStandard Deviation 7545.7
Comparison: Statistical analysis for Week 2.90% CI: [0.847, 1.267]
Comparison: Statistical analysis for Week 8.90% CI: [0.843, 1.276]
Comparison: Statistical analysis for Week 24.90% CI: [0.727, 1.151]
Secondary

BDQ PK Parameter Maxmum Plasma Concentration (Cmax) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3

This evaluates the effect of DLM on the BDQ PK parameter Cmax obtained from participants enrolled in Arms 1 and 3 (without and with co-administration of DLM). Cmax defines maximum concentration observed over the first 22 hours of the BDQ dosing interval.

Time frame: Intensive BDQ PK samples at pre-dose, 5h, 7h, 10h and 22h post-dose at weeks 2, 8 and 24

Population: Participants who took at least one dose of study treatment, and were taking study drug at the time of the PK visit.

ArmMeasureGroupValue (MEAN)Dispersion
Arm 1: BedaquilineBDQ PK Parameter Maxmum Plasma Concentration (Cmax) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Week 22434.3 ng/mLStandard Deviation 1148.4
Arm 1: BedaquilineBDQ PK Parameter Maxmum Plasma Concentration (Cmax) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Week 81455.6 ng/mLStandard Deviation 670.6
Arm 1: BedaquilineBDQ PK Parameter Maxmum Plasma Concentration (Cmax) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Week 241507.3 ng/mLStandard Deviation 495.8
Arm 2: DelamanidBDQ PK Parameter Maxmum Plasma Concentration (Cmax) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Week 22405.2 ng/mLStandard Deviation 1128.2
Arm 2: DelamanidBDQ PK Parameter Maxmum Plasma Concentration (Cmax) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Week 81477.2 ng/mLStandard Deviation 704.7
Arm 2: DelamanidBDQ PK Parameter Maxmum Plasma Concentration (Cmax) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Week 241368.2 ng/mLStandard Deviation 518.6
Comparison: Statistical analysis for Week 2.90% CI: [0.801, 1.215]
Comparison: Statistical analysis for Week 8.90% CI: [0.764, 1.251]
Comparison: Statistical analysis for Week 24.90% CI: [0.667, 1.108]
Secondary

BDQ PK Parameter Minimum Plasma Concentration (Cmin) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3

This evaluates the effect of DLM on the BDQ PK parameter Cmin obtained from participants enrolled in Arms 1 and 3 (without and with co-administration of DLM). Cmin defines minimum concentration observed over the first 22 hours of the BDQ dosing interval.

Time frame: Intensive BDQ PK samples at pre-dose, 5h, 7h, 10h and 22h post-dose at weeks 2, 8 and 24

Population: Participants who took at least one dose of study treatment, and were taking study drug at the time of the PK visit.

ArmMeasureGroupValue (MEAN)Dispersion
Arm 1: BedaquilineBDQ PK Parameter Minimum Plasma Concentration (Cmin) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Week 2796.8 ng/mLStandard Deviation 406.1
Arm 1: BedaquilineBDQ PK Parameter Minimum Plasma Concentration (Cmin) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Week 8505.9 ng/mLStandard Deviation 218.6
Arm 1: BedaquilineBDQ PK Parameter Minimum Plasma Concentration (Cmin) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Week 24653.4 ng/mLStandard Deviation 271.3
Arm 2: DelamanidBDQ PK Parameter Minimum Plasma Concentration (Cmin) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Week 2850.9 ng/mLStandard Deviation 343.8
Arm 2: DelamanidBDQ PK Parameter Minimum Plasma Concentration (Cmin) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Week 8601.9 ng/mLStandard Deviation 212.6
Arm 2: DelamanidBDQ PK Parameter Minimum Plasma Concentration (Cmin) Determined Based on BDQ Levels From Individual Participants Enrolled in Arms 1 and 3Week 24629.4 ng/mLStandard Deviation 247
Comparison: Statistical analysis for Week 2.90% CI: [0.884, 1.411]
Comparison: Statistical analysis for Week 8.90% CI: [0.989, 1.461]
Comparison: Statistical analysis for Week 24.90% CI: [0.774, 1.187]
Secondary

Changes in QTcF From Baseline

Change from baseline in QTcF, calculated as the difference between each post-baseline week and week 0. (QTcF calculated as average of 1-3 available QTcF values per visit.)

Time frame: Baseline and at weeks 2, 4, 6, 8, 10, 12, 14, 16, 18, 20, 22, 24 and 28.

Population: Participants with baseline and at least one post baseline QTcF collected at a scheduled visit while taking study TB drug(s).

ArmMeasureGroupValue (MEDIAN)
Arm 1: BedaquilineChanges in QTcF From BaselineChange from baseline to Week 2411.70 milliseconds (ms)
Arm 1: BedaquilineChanges in QTcF From BaselineChange from baseline to Week 1817.65 milliseconds (ms)
Arm 1: BedaquilineChanges in QTcF From BaselineChange from baseline to Week 129.30 milliseconds (ms)
Arm 1: BedaquilineChanges in QTcF From BaselineChange from baseline to Week 615.30 milliseconds (ms)
Arm 1: BedaquilineChanges in QTcF From BaselineChange from baseline to Week 1615.35 milliseconds (ms)
Arm 1: BedaquilineChanges in QTcF From BaselineChange from baseline to Week 1412.70 milliseconds (ms)
Arm 1: BedaquilineChanges in QTcF From BaselineChange from baseline to Week 216.70 milliseconds (ms)
Arm 1: BedaquilineChanges in QTcF From BaselineChange from baseline to Week 415.00 milliseconds (ms)
Arm 1: BedaquilineChanges in QTcF From BaselineChange from baseline to Week 2212.00 milliseconds (ms)
Arm 1: BedaquilineChanges in QTcF From BaselineChange from baseline to Week 812.00 milliseconds (ms)
Arm 1: BedaquilineChanges in QTcF From BaselineChange from baseline to Week 2813.30 milliseconds (ms)
Arm 1: BedaquilineChanges in QTcF From BaselineChange from baseline to Week 209.30 milliseconds (ms)
Arm 1: BedaquilineChanges in QTcF From BaselineChange from baseline to Week 1010.30 milliseconds (ms)
Arm 2: DelamanidChanges in QTcF From BaselineChange from baseline to Week 145.30 milliseconds (ms)
Arm 2: DelamanidChanges in QTcF From BaselineChange from baseline to Week 24.15 milliseconds (ms)
Arm 2: DelamanidChanges in QTcF From BaselineChange from baseline to Week 48.70 milliseconds (ms)
Arm 2: DelamanidChanges in QTcF From BaselineChange from baseline to Week 69.30 milliseconds (ms)
Arm 2: DelamanidChanges in QTcF From BaselineChange from baseline to Week 87.00 milliseconds (ms)
Arm 2: DelamanidChanges in QTcF From BaselineChange from baseline to Week 107.80 milliseconds (ms)
Arm 2: DelamanidChanges in QTcF From BaselineChange from baseline to Week 1210.30 milliseconds (ms)
Arm 2: DelamanidChanges in QTcF From BaselineChange from baseline to Week 167.35 milliseconds (ms)
Arm 2: DelamanidChanges in QTcF From BaselineChange from baseline to Week 1811.70 milliseconds (ms)
Arm 2: DelamanidChanges in QTcF From BaselineChange from baseline to Week 2013.65 milliseconds (ms)
Arm 2: DelamanidChanges in QTcF From BaselineChange from baseline to Week 229.00 milliseconds (ms)
Arm 2: DelamanidChanges in QTcF From BaselineChange from baseline to Week 2413.00 milliseconds (ms)
Arm 2: DelamanidChanges in QTcF From BaselineChange from baseline to Week 286.00 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidChanges in QTcF From BaselineChange from baseline to Week 1812.70 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidChanges in QTcF From BaselineChange from baseline to Week 820.30 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidChanges in QTcF From BaselineChange from baseline to Week 2424.00 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidChanges in QTcF From BaselineChange from baseline to Week 2021.00 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidChanges in QTcF From BaselineChange from baseline to Week 615.30 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidChanges in QTcF From BaselineChange from baseline to Week 213.15 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidChanges in QTcF From BaselineChange from baseline to Week 2220.85 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidChanges in QTcF From BaselineChange from baseline to Week 1421.30 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidChanges in QTcF From BaselineChange from baseline to Week 1220.30 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidChanges in QTcF From BaselineChange from baseline to Week 414.30 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidChanges in QTcF From BaselineChange from baseline to Week 1621.00 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidChanges in QTcF From BaselineChange from baseline to Week 1018.30 milliseconds (ms)
Arm 3: Bedaquiline and DelamanidChanges in QTcF From BaselineChange from baseline to Week 2817.65 milliseconds (ms)
Secondary

DLM Metabolite DM6705 PK AUC 0-11h Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3

This evaluates the effect of BDQ on the DLM Metabolite DM6705 PK parameter AUC 0-11h obtained from participants enrolled in Arms 2 and 3 (without and with co-administration of BDQ). AUC 0-11h defines area under the concentration-time curve over the first 11 hours of the DLM dosing interval.

Time frame: Intensive DLM PK samples at pre-dose, 4h, 8h, and 11h post-dose at weeks 2, 8 and 24

Population: Participants who took at least one dose of study treatment, and were taking study drug at the time of the PK visit.

ArmMeasureGroupValue (MEAN)Dispersion
Arm 1: BedaquilineDLM Metabolite DM6705 PK AUC 0-11h Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Week 2628.0 ng*h/mLStandard Deviation 188.1
Arm 1: BedaquilineDLM Metabolite DM6705 PK AUC 0-11h Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Week 8953.9 ng*h/mLStandard Deviation 395.2
Arm 1: BedaquilineDLM Metabolite DM6705 PK AUC 0-11h Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Week 24749.9 ng*h/mLStandard Deviation 420.4
Arm 2: DelamanidDLM Metabolite DM6705 PK AUC 0-11h Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Week 2621.2 ng*h/mLStandard Deviation 178.3
Arm 2: DelamanidDLM Metabolite DM6705 PK AUC 0-11h Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Week 8990.9 ng*h/mLStandard Deviation 378.1
Arm 2: DelamanidDLM Metabolite DM6705 PK AUC 0-11h Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Week 24742.5 ng*h/mLStandard Deviation 479.5
Comparison: Statistical analysis for Week 2.90% CI: [0.851, 1.138]
Comparison: Statistical analysis for Week 8.90% CI: [0.866, 1.361]
Comparison: Statistical analysis for Week 24.90% CI: [0.65, 1.322]
Secondary

DLM Metabolite DM6705 PK Parameter Cmax Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3

This evaluates the effect of BDQ on the DLM Metabolite DM6705 PK parameter Cmax obtained from participants enrolled in Arms 2 and 3 (without and with co-administration of BDQ). Cmax defines maximum concentration observed over the first 11 hours of the DLM dosing interval.

Time frame: Intensive DLM PK samples at pre-dose, 4h, 8h, and 11h post-dose at weeks 2, 8 and 24

Population: Participants who took at least one dose of study treatment, and were taking study drug at the time of the PK visit.

ArmMeasureGroupValue (MEAN)Dispersion
Arm 1: BedaquilineDLM Metabolite DM6705 PK Parameter Cmax Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Week 266.6 ng/mLStandard Deviation 18.1
Arm 1: BedaquilineDLM Metabolite DM6705 PK Parameter Cmax Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Week 899.7 ng/mLStandard Deviation 41
Arm 1: BedaquilineDLM Metabolite DM6705 PK Parameter Cmax Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Week 2482.1 ng/mLStandard Deviation 46.1
Arm 2: DelamanidDLM Metabolite DM6705 PK Parameter Cmax Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Week 264.3 ng/mLStandard Deviation 19.8
Arm 2: DelamanidDLM Metabolite DM6705 PK Parameter Cmax Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Week 8105.4 ng/mLStandard Deviation 46.2
Arm 2: DelamanidDLM Metabolite DM6705 PK Parameter Cmax Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Week 2475.6 ng/mLStandard Deviation 47.9
Comparison: Statistical analysis for Week 2.90% CI: [0.825, 1.095]
Comparison: Statistical analysis for Week 8.90% CI: [0.862, 1.354]
Comparison: Statistical analysis for Week 24.90% CI: [0.605, 1.239]
Secondary

DLM Metabolite DM6705 PK Parameter Cmin Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3

This evaluates the effect of BDQ on the DLM Metabolite DM6705 PK parameter Cmin obtained from participants enrolled in Arms 2 and 3 (without and with co-administration of BDQ). Cmin defines minimum concentration observed over the first 11 hours of the DLM dosing interval.

Time frame: Intensive DLM PK samples at pre-dose, 4h, 8h, and 11h post-dose at weeks 2, 8 and 24

Population: Participants who took at least one dose of study treatment, and were taking study drug at the time of the PK visit.

ArmMeasureGroupValue (MEAN)Dispersion
Arm 1: BedaquilineDLM Metabolite DM6705 PK Parameter Cmin Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Week 261.9 ng/mLStandard Deviation 19.3
Arm 1: BedaquilineDLM Metabolite DM6705 PK Parameter Cmin Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Week 890.6 ng/mLStandard Deviation 38.2
Arm 1: BedaquilineDLM Metabolite DM6705 PK Parameter Cmin Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Week 2475.7 ng/mLStandard Deviation 41.6
Arm 2: DelamanidDLM Metabolite DM6705 PK Parameter Cmin Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Week 258.5 ng/mLStandard Deviation 17
Arm 2: DelamanidDLM Metabolite DM6705 PK Parameter Cmin Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Week 894.4 ng/mLStandard Deviation 37.8
Arm 2: DelamanidDLM Metabolite DM6705 PK Parameter Cmin Determined Based on DLM Metabolite Levels From Individual Participants Enrolled in Arms 2 and 3Week 2471.0 ng/mLStandard Deviation 46.6
Comparison: Statistical analysis for Week 2.90% CI: [0.806, 1.094]
Comparison: Statistical analysis for Week 8.90% CI: [0.864, 1.352]
Comparison: Statistical analysis for Week 24.90% CI: [0.597, 1.253]
Secondary

DLM PK Area Under the Concentration Time Curve (AUC 0-11h) Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3

This evaluates the effect of BDQ on the DLM PK parameter AUC 0-11h obtained from participants enrolled in Arms 2 and 3 (without and with co-administration of BDQ). AUC 0-11h defines area under the concentration-time curve over the first 11 hours of the DLM dosing interval.

Time frame: Intensive DLM PK samples at pre-dose, 4h, 8h, and 11h post-dose at weeks 2, 8 and 24

Population: Participants who took at least one dose of study treatment, and were taking study drug at the time of the PK visit.

ArmMeasureGroupValue (MEAN)Dispersion
Arm 1: BedaquilineDLM PK Area Under the Concentration Time Curve (AUC 0-11h) Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Week 22789.6 ng*h/mLStandard Deviation 761.9
Arm 1: BedaquilineDLM PK Area Under the Concentration Time Curve (AUC 0-11h) Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Week 82547.6 ng*h/mLStandard Deviation 838.4
Arm 1: BedaquilineDLM PK Area Under the Concentration Time Curve (AUC 0-11h) Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Week 242473.0 ng*h/mLStandard Deviation 778.2
Arm 2: DelamanidDLM PK Area Under the Concentration Time Curve (AUC 0-11h) Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Week 22654.9 ng*h/mLStandard Deviation 724.3
Arm 2: DelamanidDLM PK Area Under the Concentration Time Curve (AUC 0-11h) Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Week 82823.2 ng*h/mLStandard Deviation 792.7
Arm 2: DelamanidDLM PK Area Under the Concentration Time Curve (AUC 0-11h) Determined Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 2 and 3Week 242324.9 ng*h/mLStandard Deviation 987.3
Comparison: Statistical analysis for Week 2.90% CI: [0.825, 1.096]
Comparison: Statistical analysis for Week 8.90% CI: [0.948, 1.362]
Comparison: Statistical analysis for Week 24.90% CI: [0.727, 1.109]
Secondary

DLM PK Parameter Cmax Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3

This evaluates the effect of BDQ on the DLM PK parameter Cmax obtained from participants enrolled in Arms 2 and 3 (without and with co-administration of BDQ). Cmax defines maximum concentration observed over the first 11 hours of the DLM dosing interval.

Time frame: Intensive DLM PK samples at pre-dose, 4h, 8h, and 11h post-dose at weeks 2, 8 and 24

Population: Participants who took at least one dose of study treatment, and were taking study drug at the time of the PK visit.

ArmMeasureGroupValue (MEAN)Dispersion
Arm 1: BedaquilineDLM PK Parameter Cmax Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Week 2317.8 ng/mLStandard Deviation 88.7
Arm 1: BedaquilineDLM PK Parameter Cmax Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Week 8294.1 ng/mLStandard Deviation 100
Arm 1: BedaquilineDLM PK Parameter Cmax Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Week 24290.3 ng/mLStandard Deviation 81.6
Arm 2: DelamanidDLM PK Parameter Cmax Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Week 2298.3 ng/mLStandard Deviation 84.2
Arm 2: DelamanidDLM PK Parameter Cmax Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Week 8320.9 ng/mLStandard Deviation 98.4
Arm 2: DelamanidDLM PK Parameter Cmax Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Week 24259.0 ng/mLStandard Deviation 102.8
Comparison: Statistical analysis for Week 2.90% CI: [0.81, 1.084]
Comparison: Statistical analysis for Week 8.90% CI: [0.929, 1.318]
Comparison: Statistical analysis for Week 24.90% CI: [0.703, 1.043]
Secondary

DLM PK Parameter Cmin Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3

This evaluates the effect of BDQ on the DLM PK parameter Cmin obtained from participants enrolled in Arms 2 and 3 (without and with co-administration of BDQ). Cmin defines minimum concentration observed over the first 11 hours of the DLM dosing interval.

Time frame: Intensive DLM PK samples at pre-dose, 4h, 8h, and 11h post-dose at weeks 2, 8 and 24

Population: Participants who took at least one dose of study treatment, and were taking study drug at the time of the PK visit.

ArmMeasureGroupValue (MEAN)Dispersion
Arm 1: BedaquilineDLM PK Parameter Cmin Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Week 2224.8 ng/mLStandard Deviation 59
Arm 1: BedaquilineDLM PK Parameter Cmin Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Week 8198.2 ng/mLStandard Deviation 64.3
Arm 1: BedaquilineDLM PK Parameter Cmin Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Week 24220.9 ng/mLStandard Deviation 78.9
Arm 2: DelamanidDLM PK Parameter Cmin Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Week 2206.8 ng/mLStandard Deviation 64.8
Arm 2: DelamanidDLM PK Parameter Cmin Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Week 8217.2 ng/mLStandard Deviation 64.6
Arm 2: DelamanidDLM PK Parameter Cmin Determined Based on DLM Levels From Individual Participants Enrolled in Arms 2 and 3Week 24182.2 ng/mLStandard Deviation 78.5
Comparison: Statistical analysis for Week 2.90% CI: [0.778, 1.049]
Comparison: Statistical analysis for Week 8.90% CI: [0.944, 1.315]
Comparison: Statistical analysis for Week 24.90% CI: [0.639, 1.012]
Secondary

N-monodesmethyl Metabolite of BDQ PK Parameter AUC 0-22h Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3

This evaluates the effect of DLM on the N-monodesmethyl Metabolite of BDQ PK parameter AUC 0-22h obtained from participants enrolled in Arms 1 and 3 (without and with co-administration of DLM). AUC 0-22h defines area under the concentration-time curve over the period of 22 hours post-dose.

Time frame: Intensive BDQ PK samples at pre-dose, 5h, 7h, 10h and 22h post-dose at Weeks 2, 8 and 24

Population: Participants who took at least one dose of study treatment, and were taking study drug at the time of the PK visit.

ArmMeasureGroupValue (MEAN)Dispersion
Arm 1: BedaquilineN-monodesmethyl Metabolite of BDQ PK Parameter AUC 0-22h Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Week 28435.5 ng*h/mLStandard Deviation 3220.1
Arm 1: BedaquilineN-monodesmethyl Metabolite of BDQ PK Parameter AUC 0-22h Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Week 85067.5 ng*h/mLStandard Deviation 2017.6
Arm 1: BedaquilineN-monodesmethyl Metabolite of BDQ PK Parameter AUC 0-22h Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Week 244771.4 ng*h/mLStandard Deviation 1577.9
Arm 2: DelamanidN-monodesmethyl Metabolite of BDQ PK Parameter AUC 0-22h Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Week 28713.4 ng*h/mLStandard Deviation 2858.9
Arm 2: DelamanidN-monodesmethyl Metabolite of BDQ PK Parameter AUC 0-22h Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Week 84963.4 ng*h/mLStandard Deviation 1847.6
Arm 2: DelamanidN-monodesmethyl Metabolite of BDQ PK Parameter AUC 0-22h Calculated Based on Intensive PK Samples Obtained From Individual Participants Enrolled in Arms 1 and 3Week 244033.5 ng*h/mLStandard Deviation 1978.7
Comparison: Statistical analysis for Week 2.90% CI: [0.881, 1.248]
Comparison: Statistical analysis for Week 8.90% CI: [0.823, 1.165]
Comparison: Statistical analysis for Week 24.90% CI: [0.638, 1.025]
Secondary

N-monodesmethyl Metabolite of BDQ PK Parameter Cmax Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3

This evaluates the effect of DLM on the BDQ Metabolite N-monodesmethyl BDQ PK parameter Cmax obtained from participants enrolled in Arms 1 and 3 (without and with co-administration of DLM). Cmax defines maximum concentration observed over the first 22 hours of the BDQ dosing interval.

Time frame: Intensive BDQ Metabolite PK samples at pre-dose, 5h, 7h, 10h and 22h post-dose at weeks 2, 8 and 24

Population: Participants who took at least one dose of study treatment, and were taking study drug at the time of the PK visit.

ArmMeasureGroupValue (MEAN)Dispersion
Arm 1: BedaquilineN-monodesmethyl Metabolite of BDQ PK Parameter Cmax Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Week 2404.8 ng/mLStandard Deviation 143.7
Arm 1: BedaquilineN-monodesmethyl Metabolite of BDQ PK Parameter Cmax Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Week 8248.5 ng/mLStandard Deviation 95.4
Arm 1: BedaquilineN-monodesmethyl Metabolite of BDQ PK Parameter Cmax Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Week 24232.9 ng/mLStandard Deviation 68.6
Arm 2: DelamanidN-monodesmethyl Metabolite of BDQ PK Parameter Cmax Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Week 2429.8 ng/mLStandard Deviation 139.8
Arm 2: DelamanidN-monodesmethyl Metabolite of BDQ PK Parameter Cmax Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Week 8241.5 ng/mLStandard Deviation 87.2
Arm 2: DelamanidN-monodesmethyl Metabolite of BDQ PK Parameter Cmax Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Week 24196.8 ng/mLStandard Deviation 92.5
Comparison: Statistical analysis for Week 2.90% CI: [0.903, 1.263]
Comparison: Statistical analysis for Week 8.90% CI: [0.82, 1.155]
Comparison: Statistical analysis for Week 24.90% CI: [0.656, 0.983]
Secondary

N-monodesmethyl Metabolite of BDQ PK Parameter Cmin Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3

This evaluates the effect of DLM on the N-monodesmethyl Metabolite of BDQ PK parameter Cmin obtained from participants enrolled in Arms 1 and 3 (without and with co-administration of DLM). Cmin defines minimum concentration observed over the first 22 hours of the BDQ dosing interval.

Time frame: Intensive BDQ Metabolite PK samples at pre-dose, 5h, 7h, 10h and 22h post-dose at weeks 2, 8 and 24

Population: Participants who took at least one dose of study treatment, and were taking study drug at the time of the PK visit.

ArmMeasureGroupValue (MEAN)Dispersion
Arm 1: BedaquilineN-monodesmethyl Metabolite of BDQ PK Parameter Cmin Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Week 2353.3 ng/mLStandard Deviation 137.8
Arm 1: BedaquilineN-monodesmethyl Metabolite of BDQ PK Parameter Cmin Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Week 8200.0 ng/mLStandard Deviation 81.1
Arm 1: BedaquilineN-monodesmethyl Metabolite of BDQ PK Parameter Cmin Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Week 24204.0 ng/mLStandard Deviation 62.8
Arm 2: DelamanidN-monodesmethyl Metabolite of BDQ PK Parameter Cmin Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Week 2361.6 ng/mLStandard Deviation 122.8
Arm 2: DelamanidN-monodesmethyl Metabolite of BDQ PK Parameter Cmin Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Week 8204.7 ng/mLStandard Deviation 76.3
Arm 2: DelamanidN-monodesmethyl Metabolite of BDQ PK Parameter Cmin Determined Based on BDQ Metabolite Levels From Individual Participants Enrolled in Arms 1 and 3Week 24174.0 ng/mLStandard Deviation 82.1
Comparison: Statistical analysis for Week 2.90% CI: [0.864, 1.258]
Comparison: Statistical analysis for Week 8.90% CI: [0.858, 1.235]
Comparison: Statistical analysis for Week 24.90% CI: [0.657, 0.993]
Secondary

Percentage of Participants Who Died

Among participants who took at least one dose of study TB treatment, percentage of participants who died on or before week 24. Note that the all-cause mortality includes deaths that occurred at any time during treatment or follow-up through week 128.

Time frame: From initiation of study TB treatment (week 0) to week 24

Population: Participants who took at least one dose of study TB treatment.

ArmMeasureValue (NUMBER)
Arm 1: BedaquilinePercentage of Participants Who Died0 Percentage of participants
Arm 2: DelamanidPercentage of Participants Who Died0 Percentage of participants
Arm 3: Bedaquiline and DelamanidPercentage of Participants Who Died0 Percentage of participants
Secondary

Percentage of Participants Who Discontinued Study TB Drug(s) For Any Reason

Percentage of participants who discontinued study TB drug(s) for any reason

Time frame: From initiation of study TB treatment (week 0) to week 24

Population: Participants who took at least one dose of study TB treatment.

ArmMeasureValue (NUMBER)
Arm 1: BedaquilinePercentage of Participants Who Discontinued Study TB Drug(s) For Any Reason11 Percentage of participants
Arm 2: DelamanidPercentage of Participants Who Discontinued Study TB Drug(s) For Any Reason19 Percentage of participants
Arm 3: Bedaquiline and DelamanidPercentage of Participants Who Discontinued Study TB Drug(s) For Any Reason22 Percentage of participants
Secondary

Percentage of Participants With an Increase in QTcF From Baseline of Greater Than 60 Milliseconds (ms)

Participants who experienced QTcF increase from baseline greater than 60 ms at least once at any time from week 2 to 24. QTcF calculated as average of 1-3 available QTcF values per visit.

Time frame: Baseline and at weeks 2, 4, 6, 8, 10, 12, 14, 16, 18, 20, 22 and 24

Population: Participants who took at least one dose of study TB treatment.

ArmMeasureValue (NUMBER)
Arm 1: BedaquilinePercentage of Participants With an Increase in QTcF From Baseline of Greater Than 60 Milliseconds (ms)4 Percentage of participants
Arm 2: DelamanidPercentage of Participants With an Increase in QTcF From Baseline of Greater Than 60 Milliseconds (ms)0 Percentage of participants
Arm 3: Bedaquiline and DelamanidPercentage of Participants With an Increase in QTcF From Baseline of Greater Than 60 Milliseconds (ms)7 Percentage of participants
Secondary

Percentage of Participants With an Occurrence of Grade 3 or Higher Adverse Event

Participants with an occurrence of an adverse event (laboratory value, sign/symptom, diagnosis) of grade 3 or 4. Severity grading based on DAIDS AE Grading Table Version 2.0. Participants were counted once at the highest grade (grade 3 or grade 4).

Time frame: From initiation of study TB treatment (week 0) to week 24

Population: Participants who took at least one dose of study TB treatment.

ArmMeasureGroupValue (NUMBER)
Arm 1: BedaquilinePercentage of Participants With an Occurrence of Grade 3 or Higher Adverse EventGrade 3 adverse event36 Percentage of participants
Arm 1: BedaquilinePercentage of Participants With an Occurrence of Grade 3 or Higher Adverse EventGrade 4 adverse event4 Percentage of participants
Arm 2: DelamanidPercentage of Participants With an Occurrence of Grade 3 or Higher Adverse EventGrade 3 adverse event11 Percentage of participants
Arm 2: DelamanidPercentage of Participants With an Occurrence of Grade 3 or Higher Adverse EventGrade 4 adverse event11 Percentage of participants
Arm 3: Bedaquiline and DelamanidPercentage of Participants With an Occurrence of Grade 3 or Higher Adverse EventGrade 3 adverse event19 Percentage of participants
Arm 3: Bedaquiline and DelamanidPercentage of Participants With an Occurrence of Grade 3 or Higher Adverse EventGrade 4 adverse event19 Percentage of participants
Secondary

Percentage of Participants With an Occurrence of QTcF >480 and ≤500 Milliseconds (ms)

Participants who experienced QTcF \>480 and ≤500 ms at least once at any time from week 2 to 24. QTcF calculated as average of 1-3 available QTcF values per visit.

Time frame: At weeks 2, 4, 6, 8, 10, 12, 14, 16, 18, 20, 22 and 24

Population: Participants who took at least one dose of study TB drug(s).

ArmMeasureValue (NUMBER)
Arm 1: BedaquilinePercentage of Participants With an Occurrence of QTcF >480 and ≤500 Milliseconds (ms)0 Percentage of participants
Arm 2: DelamanidPercentage of Participants With an Occurrence of QTcF >480 and ≤500 Milliseconds (ms)0 Percentage of participants
Arm 3: Bedaquiline and DelamanidPercentage of Participants With an Occurrence of QTcF >480 and ≤500 Milliseconds (ms)0 Percentage of participants
Secondary

Percentage of Participants With an Occurrence of QTcF Greater Than 500 Milliseconds (ms)

Participants who experienced QTcF greater than 500 ms at least once at any time from week 2 to 24. QTcF calculated as average of 1-3 available QTcF values per visit.

Time frame: At weeks 2, 4, 6, 8, 10, 12, 14, 16, 18, 20, 22 and 24

Population: Participants who took at least one dose of study TB treatment.

ArmMeasureValue (NUMBER)
Arm 1: BedaquilinePercentage of Participants With an Occurrence of QTcF Greater Than 500 Milliseconds (ms)0 Percentage of participants
Arm 2: DelamanidPercentage of Participants With an Occurrence of QTcF Greater Than 500 Milliseconds (ms)0 Percentage of participants
Arm 3: Bedaquiline and DelamanidPercentage of Participants With an Occurrence of QTcF Greater Than 500 Milliseconds (ms)0 Percentage of participants
Secondary

Percentage of Participants With an Occurrence of QTcF Increase From Baseline of >30 and ≤60 Milliseconds (ms)

Participants who experienced QTcF increase from baseline of \>30 and ≤60 ms at least once at any time from week 2 to 24. QTcF calculated as average of 1-3 available QTcF values per visit.

Time frame: Baseline and at weeks 2, 4, 6, 8, 10, 12, 14, 16, 18, 20, 22 and 24

Population: Participants who took at least one dose of study treatment.

ArmMeasureValue (NUMBER)
Arm 1: BedaquilinePercentage of Participants With an Occurrence of QTcF Increase From Baseline of >30 and ≤60 Milliseconds (ms)32 Percentage of participants
Arm 2: DelamanidPercentage of Participants With an Occurrence of QTcF Increase From Baseline of >30 and ≤60 Milliseconds (ms)41 Percentage of participants
Arm 3: Bedaquiline and DelamanidPercentage of Participants With an Occurrence of QTcF Increase From Baseline of >30 and ≤60 Milliseconds (ms)37 Percentage of participants

Source: ClinicalTrials.gov · Data processed: Feb 24, 2026