Linezolid, Aspirin and Enhanced Dose Rifampicin in HIV-TBM

HIV-1-infection Clinical Trial

— LASER-TBM  

Official title:

Phase IIA Trial of the Safety and Tolerability of Increased Dose Rifampicin and Adjunctive Linezolid With or Without Aspirin, for HIV-associated Tuberculous Meningitis

Clinical Trial Details — Status: Completed

Administrative data

• NCT number: NCT03927313
• Other study ID #: LASER-TBM
• Status: Completed
• Phase: Phase 2
• Start date: June 12, 2019
• Est. completion date: March 31, 2021

Study information

• Verified date: September 2021
• Source: University of Cape Town
• Contact: n/a
• Is FDA regulated: No
• Study type: Interventional

Clinical Trial Summary

LASER-TBM is a parallel group, randomized, multi-arm phase IIa trial evaluating the safety of increased dose rifampicin (RIF) plus linezolid (LZD), with or without aspirin (ASA), for the treatment of HIV-infected adults with tuberculous meningitis (TBM). The study will recruit 100 HIV-infected adults with TBM across four sites in South Africa.

The primary endpoint is the occurrence of solicited treatment-related adverse events.

Secondary endpoints include death and disability (including neurocognitive impairment), radiological outcomes, and the occurrence of immune reconstitution inflammatory syndrome (IRIS).

A nested pharmacokinetic (PK) substudy aims to:

1. Describe the plasma and cerebrospinal fluid (CSF) PK of LZD and high dose RIF.

2. Evaluate the relationship between drug exposures, toxicity and efficacy.

3. Compare exposures between intravenous and oral RIF administration.

4. Investigate the impact of high dose RIF on LZD and dolutegravir (DTG).

Description:

HIV-1 infected adults with newly-diagnosed TBM (n = 100) will be recruited from four public-sector hospitals in Cape Town and Port Elizebeth, South Africa. Participants will be randomised across two experimental (n = 30 each) and one standard of care (n = 40) arms. Treatment will be provided in all arms for 56 days, after which participants will be referred back to public sector facilities to complete standard therapy for HIV-associated TBM.

The primary objective of the study is to investigate the safety of enhanced antimicrobial therapy including increased dose RIF and LZD with or without adjunctive aspirin added to standard therapy for TBM in HIV-1 infected adults.

Secondary objectives are;

1. To determine cerebrospinal fluid M.tb culture positivity and Gene Xpert® Ultra positivity at baseline and at 3 and 28 days post treatment by allocation.

2. To evaluate the effect of aspirin and enhanced tuberculosis treatment on the incidence of immune reconstitution syndrome in participants starting antiretroviral therapy.

3. To evaluate the effect of high dose rifampicin and linezolid, with and without aspirin on the transcriptional signature derived from whole blood and cerebrospinal fluid RNA sequencing, as well as the metabolomic and proteomic profiles, in tuberculous meningitis.

4. To evaluate the effect of high dose rifampicin and linezolid with and without aspirin on central nervous system imaging in conjunction with clinical, immunological and transcriptional profiling.

5. To store biological samples for future analysis of potential biomarkers of treatment efficacy and/or novel diagnostic assays.

6. To determine i) whether host genotype, including LTA4H genotype, influences therapeutic effect of aspirin in HIV-TBM and ii) the pharmacogenetic influence on rifampicin and linezolid exposures and toxicity.

All participants will receive antitubercular chemotherapy and corticosteroids as standard of care as per national South African guidelines. Participants allocated to experimental arms 2 and 3 will receive additional rifampicin (total oral dose 35 mg/kg/day) plus oral linezolid 1200mg daily for the first 28 days, reduced to 600 mg daily for the next 28 days. Those randomized to experimental arm 3 will also receive oral aspirin 1000 mg daily.

All consenting LASER-TBM participants in experimental arms (n = 60) will undergo a second randomisation to receive either oral (35mg/kg) or IV (20mg/kg) rifampicin at the time of study entry. This sub-study is powered to demonstrate bioequivalence at day 3 of administration, after which all participants will be continued on oral rifampicin dosed at 35mg/kg.

Trial participation will be for 180 days post-randomization: primary safety endpoints and secondary efficacy endpoints will be evaluated at day 56; additional secondary endpoints will be evaluated at day 180.

There are seven scheduled study visits. The first six of thee will occur within the first 56 days, with an additional structured interview at 6 months. All visits will involve a clinical assessment including specified clinical outcome measures to assess functional and cognitive disability. Phlebotomy will be performed at study visits within the first 56 days to monitor for pre-specified parameters of drug safety (haematology, biochemistry) as well as to collect blood for downstream transcriptomic, proteomic and metabolomic analysis. Lumbar puncture will take place at day 3 and day 28. Cerebrospinal fluid will be analysed for Mycobacterium tuberculosis culture and Gene Xpert® Ultra cycle threshold values. Cerebrospinal fluid (CSF) will be stored for downstream transcriptomic, proteomic and metabolomic analysis. Baseline and day 56 brain imaging will be performed in all study participants.

All enrolled participants will undergo sparse plasma PK sampling at the Day 28 and Day 56 visits.

Cerebrospinal fluid (CSF) will be collected from all participants for determination of linezolid and rifampicin concentrations on Days 3 and 28. The timing of the Day 3 lumbar puncture will be randomised to intervals of 1 - 3, 3 - 6, 6 - 10, and 24 hours after observed antitubercular drug dosing in order to construct a concentration-time profile for the population. A single sample will be collected at each time interval. A second lumbar puncture will take place at the Day 28 visit, to coincide with the 4-hour plasma PK sample.

All participants (n=100) will be offered participation in the intensive sampling component of the PK sub-study at the time of randomization to the main study. Intensive plasma sampling will take place at the Day 3 study visit. Serial venous blood samples will be collected through a peripheral intravenous catheter pre-dose, and at 0.5, 1, 2, 3, 6, 8 - 10, and 24 hours after witnessed drug intake and an overnight fast. Sparse sampling will be performed at Day 3 for participants who decline intensive sampling or in whom this fails.

Recruitment information / eligibility

• Status: Completed
• Enrollment: 52
• Est. completion date: March 31, 2021
• Est. primary completion date: March 30, 2021
• Accepts healthy volunteers: No
• Gender: All
• Age group: 18 Years and older

Eligibility

Inclusion Criteria:

• HIV-1 seropositivity by rapid test, confirmed by enzyme-linked immunosorbent assay (regardless of Antiretroviral Therapy (ART) status);

• Age 18 years or older;

• Tuberculous meningitis defined as 'possible', 'probable' or 'definite' as per published case definitions

Exclusion Criteria:

• Rifampicin-resistant M. tb detected in any microbiological specimen;

• History of allergy or hypersensitivity to H, E, R and Z, LZD or ASA;

• Received more than 5 days of antitubercular therapy in the 30 days prior to screening;

• Received a dose of ASA or any other NSAID within 2 weeks of screening;

• CSF unobtainable by lumbar puncture or another procedure;

• Evidence of bacterial or cryptococcal meningitis;

• Severe concurrent uncontrolled opportunistic infection including but not limited to active cytomegalovirus-associated disease, Kaposi sarcoma, Pneumocystis jirovecii pneumonia, HIV related or unrelated malignancy or gastrointestinal bleeding;

• Any other form of immunosuppressive therapy including antineoplastic and biologic agents apart from corticosteroids;

• Is pregnant in the third trimester;

• Peripheral neuropathy scoring Grade 3 or above on Brief Peripheral Neuropathy Score

• Any disease or condition in which the use of the standard TB drugs or any of their components is contraindicated, including but not limited to allergy to any TB drug or their components;

• The presence of one or more of the following:

• Estimated glomerular filtration rate (eGFR) < 20ml/min/1.73m2 (using the Cockcroft-Gault equation)

• International normalised ration (INR) > 1.4 and/or clinical evidence of liver failure or decompensated cirrhosis

• Hemoglobin < 8.0 g/dL

• Platelets < 50 x109 /L

• Neutrophils < 0.5 x 109 cells/L;

• The patient has any disease or condition in which any of the medicinal products listed in the section pertaining to prohibited medication is used and cannot be safely stopped;

• The patient has a known or suspected, current or history of drug abuse, within the past 2 years, that is, in the opinion of the investigators, sufficient to compromise the safety or cooperation of the patient.

Related Conditions & MeSH terms

• HIV-1-infection
• Meningitis
• Tuberculosis
• Tuberculosis Meningitis
• Tuberculosis, Meningeal

Intervention

Drug:
• Linezolid
For both experimental arms: 1.2g linezolid 28 days, followed by 600mg linezolid for 28 days
• High dose rifampicin
For both experimental arms: additional 25mg/kg (making a total of 35mg/kg) rifampicin, for the first 56 days of treatment
• Aspirin
For only one of the experimental arms: 1000mg of aspirin daily for 56 days.
• Standard of Care anti-tuberculous therapy
10mg/kg oral rifampicin, 5mg/kg oral isoniazid, 15mg/kg oral ethambutol, 25mg/kg oral pyrazinamide daily for 56 days.
• Dexamethasone
Dexamethasone according to doses of Thwaites criteria for the first 8 weeks of anti-tuberculous treatment. Doses differ according to participants Medical Research Council (MRC) grade. Given orally if participant can swallow and intravenously if they cannot.

Locations

Country	Name	City	State
South Africa	Groote Schuur Hospital	Cape Town	Western Cape
South Africa	Mitchells Plain Hospital	Cape Town	Western Cape
South Africa	New Somerset Hospital	Cape Town	Western Cape
South Africa	Livingstone Hospital	Port Elizabeth	Eastern Cape

Sponsors (1)

Lead Sponsor	Collaborator
University of Cape Town

Country where clinical trial is conducted

South Africa, 

Outcome

Type	Measure	Description	Time frame	Safety issue
Primary	Number of participants in each arm who develop treatment related adverse events (AEs).	The amount of participants who develop any of the following treatment related adverse events by the time they have been on treatment for 56 days will be counted: Peripheral neuropathy, optic neuropathy, anaemia, neutropaenia, thrombocytopaenia, upper gastro-intestinal haemorrhage, intracerebral haemorrhage, drug-induced liver injury.	56 days
Secondary	Death and disability after 56 days on treatment.	A comparison will be made of the proportion of participants in each arm who died, and their grade of disability will be compared according to Modified Rankin Scoring.	56 days
Secondary	Death at day 56 and day 180.	In all arms: the number of participants who have died at Day 56 will be compared to those that have died at Day 180.	180 days
Secondary	Number of participants who are disabled.	Comparison of level of disability of participants at 56 and 180 days, stratifying by Medical Research Council grade.	180 days
Secondary	Number of participants who develop Grade 3 or Grade 4 adverse events (AEs).	In all 3 arms: comparison of the number of participants who develop Grade 3 or Grade 4 adverse events (according to Division of AIDS (DAIDS) criteria) by the time they have been on treatment or 56 days.	56 days
Secondary	Number of participants in whom experimental drugs had to be stopped.	At 56 days on treatment, the number of participants in the experimental arms in whom rifampicin, linezolid and/or aspirin had to be stopped.	56 days
Secondary	Linezolid toxicity	To note the presence of the following adverse events in all participants in the experimental arms: peripheral neuropathy, optic neuropathy, anaemia, neutropaenia, thrombocytopaenia and hyperlactataemia.	56 days
Secondary	Major bleeding events.	To note at 6 months, the amount of participants who develop upper gastro-intestinal or intra-cerebral haemorrhage after receiving 1000mg daily aspirin as part of the trial.	180 days
Secondary	Cerebrospinal fluid culture conversion.	To compare in the different arms, between lumbar punctures done at day 3 and day 28, the time to automated liquid culture positivity and Gene-Xpert ultra threshold values (for mycobacterium tuberculosis) of cerebrospinal fluid.	Day 28 and day 56
Secondary	The occurrence of TBM-immune reconstitution inflammatory syndrome	The amount of participants in all 3 arms who develop paradoxical tuberculosis immune reconstitution, as defined by th modified INSHI criteria.	56 days
Secondary	Changes on brain imaging	To compare at day 56, in participants who had brain imaging at baseline, changes in brain imaging at day 56.	Day 56