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RecruitingPhase 2Phase 3NCT04310930

Finding the Optimal Regimen for Mycobacterium Abscessus Treatment

Finding the Optimal Regimen for Mycobacterium Abscessus Treatment (FORMaT)

Sponsor

The University of Queensland

Enrollment

300 participants

Start Date

Mar 2, 2020

Study Type

INTERVENTIONAL

Conditions

Pulmonary Disease Due to Mycobacteria (Diagnosis)

Summary

Mycobacterium abscessus (MABS) is a group of rapid-growing, multi-drug resistant non-tuberculous mycobacteria (NTM) causing infections in humans. MABS pulmonary disease (MABS-PD) can result in significant morbidity, increased healthcare utilisation, accelerated lung function decline, impaired quality of life, more challenging lung transplantation, and increased mortality. While the overall numbers affected is small, the prevalence of infections is increasing worldwide. The Finding the Optimal Regimen for Mycobacterium abscessus Treatment (FORMaT) trial aims to produce high quality evidence for the best treatment regimens to maximise health outcomes and minimise toxicity and treatment burden, as well as developing biomarkers (serology, gene expression signatures, and radiology) to guide decisions for starting treatment and measuring disease severity in patients with MABS PD.

Eligibility

Inclusion Criteria21

  • Eligibility criteria for the FORMaT trial can be applied at two levels:
  • Eligibility into the Intervention Program, or;
  • Eligibility into the Observational Cohort.
  • Potential participants can only be enrolled in either the Intervention Program or the Observational Cohort at any one time. Provided the eligibility criteria are met, potential participants may either:
  • Enrol directly into the Intervention Program, or;
  • Eligibility into the FORMaT trial will be assessed at screening. Observational Cohort participants who go on to meet the Intervention Program eligibility criteria can transition from the Observational Cohort to the Intervention Program.
  • Positive MABS-PD diagnosis meeting all three American Thoracic Society clinical, radiological and microbiological diagnostic criteria for MABS-PD. Defined as:
  • Clinical: Pulmonary symptoms and exclusion of other diagnoses.
  • Radiological: Nodular or cavitary opacities on chest radiograph or a chest high-resolution computed tomography (HRCT) scan showing multifocal bronchiectasis with multiple small nodules.
  • Microbiological: MABS positive culture results from at least two separate expectorated sputum samples.
  • or Positive culture results from at least one bronchial wash or lavage. or Transbronchial or other lung biopsy with mycobacterial histopathologic features (granulomatous inflammation or acid-fast bacilli (AFB)) and positive culture for NTM or biopsy showing mycobacterial histopathologic features (granulomatous inflammation or AFB) and one or more sputum or bronchial washes that are culture positive for NTM.
  • Screening samples must be collected within the timeframes stated in the relevant appendix.
  • Male or female participants of any age.
  • Participant has not received treatment for MABS-PD in the 12 months preceding assessment of eligibility or as specified in the relevant appendix (this includes drugs prescribed for the treatment of other mycobacteria and/or other indications that may have activity against MABS, as specified in the FORMaT Prohibited Drug List Standard Operating Procedure (SOP)).
  • Informed consent signed by participant or parent/legal guardian if participant is under 18 years of age.
  • Ability to comply with study visits, therapies and study procedures as judged by the site investigator.
  • To be eligible to participate in the Observational Cohort the following criteria must be met:
  • Male and female participants of any age with at least one positive respiratory culture for MABS.
  • Informed consent signed by participant or parent/legal guardian if participant is under 18 years of age.
  • Ability to comply with study visits and study procedures as judged by the site investigator.
  • Appendix specific sub-studies and integrated studies Appendix specific sub-studies and integrated studies may have additional eligibility criteria which are described in each of the relevant appendices.

Exclusion Criteria6

  • Participants receiving current treatment for MABS (this includes drugs prescribed for the treatment of other mycobacteria and/or other indications that may have activity against MABS, as specified in the FORMaT Prohibited Drug List SOP), except for participants taking azithromycin as part of routine treatment for CF or chronic infection-related pulmonary disease, or as specified in the relevant appendix.
  • Participants who have a QTc interval of >500 milliseconds (QT interval corrected based on Fridericia method).
  • Participants who are pregnant or planning to continue breast feeding.
  • Known hypersensitivity or contraindication to any of the therapies for which no alternative option(s) have been provided.
  • Potential participants will be ineligible to participate in the Observational Cohort if any of the following criterion are met:
  • Receiving active treatment for MABS within the previous 12 months (this includes drugs prescribed for the treatment of other mycobacteria and/or other indications that may have activity against MABS, as specified in the FORMaT Prohibited Drug List SOP, except for participants taking azithromycin as part of routine treatment for CF or chronic infection-related pulmonary disease).

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Interventions

DRUGAmikacin

Adults: Intravenous amikacin 5mg/kg once daily or 7.5mg/kg twice daily or 20-25 mg/kg thrice weekly. Children:Intravenous amikacin 15-30 mg/kg once daily, maximum dose 1500mg

DRUGTigecycline

Adults: Intravenous Tigecycline 25 mg increasing by 5 mg every two doses until either maximum dose reached (50mg) or until patient is unable to tolerate twice daily. Children (≥8 years of age) intravenous tigecycline: Day 1- 0.6mg/kg twice daily to a maximum of 25mg. Day 2- 0.6mg/kg (maximum 25mg) in the morning, 1.2 mg/kg (maximum 50mg) at night. Day 3- 1.2mg/kg (maximum 50 mg) twice daily

DRUGImipenem

Adults: Intravenous Imipenem (≥50kg) 500mg twice daily (\<50kg) 15 mg/kg twice daily. Children: intravenous imipenem Day 1- 2- 25mg/kg (maximum 1g) twice daily. DAY 3- 25mg/kg (maximum 1g) four times daily (drop to 3 if not tolerated).

DRUGCefoxitin

Adults: If imipenem is poorly tolerated intravenous cefoxitin 200 mg/kg thrice daily. Children: if imipenem is poorly tolerated intravenous cefoxitin 50mg/kg (maximum 4g) four times daily.

DRUGAzithromycin

Adults: Oral azithromycin 500mg (≥40kg) once daily, (\<40kg) 250mg once daily.During consolidaiton: 500mg (≥40kg) thrice weekly, (\<40kg) 250mg thrice weekly. Children: Oral azithromycin:10mg/kg (maximum 500mg) once daily. During consolidation 10mg/kg once daily maximum 500mg.

DRUGClarithromycin

Adult: If azithromycin is poorly tolerated use oral clarithromycin 500mg twice daily.Children: If azithromycin is poorly tolerated use oral clarithromycin. In children 1 month old- 11years of age the following dosing applies: \<8kg: 7.5mg/kg twice daily, maximum dose 62.5mg, 8-11kg: 62.5mg twice daily, maximum dose 62.5mg, 12-19 kg: 125mg twice daily, maximum dose 125mg, 20-29 kg: 187.5mg twice daily, maximum dose 187.5mg, 30-40 kg: 250mg twice daily, maximum dose 250mg, Children 12-18 years of age: 500 mg twice daily

DRUGClofazimine

Adult: Oral clofazimine 100mg once daily. Children: Oral clofazimine: 3-5mg/kg once daily. Maximum dose of 50mg once daily if \<40kg or 100mg if ≥40kg once daily.

DRUGEthambutol

Adults: with confirmed mixed NTM infections (slow growers + MABS) oral ethambutol can be added at either 15 mg/kg once daily or 25mg/kg thrice weekly. Children with confirmed mixed NTM infections (slow growers + MABS) oral ethambutol can be added at 20 mg/kg once daily.

DRUGAmikacin

adult: Inhaled amikacin 500mg twice daily. Children: Inhaled amikacin 500mg twice daily

DRUGLinezolid

Adult: during consolidation in combination with one to three oral antibiotics (co-trimoxazole, doxycycline, moxifloxacin, bedaquiline or rifabutin) guided by participant susceptibility and tolerance. Oral linezolid 600mg once daily. Children: during consolidation in combination with one to three oral antibiotics (co-trimoxazole, doxycycline, moxifloxacin or rifabutin) guided by participant susceptibility and tolerance. Age 1 week - 9 years 10mg/kg twice daily maximum dose of 300mg. Age 10-12 years 10mg/kg twice daily maximum dose of 600mg. \>12 years 600mg once daily.

DRUGco-trimoxazole

Adult: during consolidation in combination with one to three oral antibiotics (co-trimoxazole, doxycycline, moxifloxacin, bedaquiline or rifabutin) guided by participant susceptibility and tolerance. Oral Co-trimoxazole (TMP-SMX) 160/800mg twice daily. Children: During consolidation in combination with one to three oral antibiotics (co-trimoxazole, doxycycline, moxifloxacin or rifabutin) guided by participant susceptibility and tolerance. Oral co-trimoxazole 5mg TMP/kg maximum dose of 160mg TMP/ 800mg SMX twice daily.

DRUGDoxycycline

Adult: during consolidation in combination with one to three oral antibiotics (co-trimoxazole, doxycycline, moxifloxacin, bedaquiline or rifabutin) guided by participant susceptibility and tolerance. Oral doxycycline 100mg once daily. Children: During consolidation in combination with one to three oral antibiotics (co-trimoxazole, doxycycline, moxifloxacin or rifabutin) guided by participant susceptibility and tolerance. Oral doxycycline (ages ≥ 8 years) 2mg/kg once daily maximum dose 100mg.

DRUGMoxifloxacin

Adult: during consolidation in combination with one to three oral antibiotics (co-trimoxazole, doxycycline, moxifloxacin, bedaquiline or rifabutin) guided by participant susceptibility and tolerance. Oral moxifloxacin 400mg once daily. Children: During consolidation in combination with one to three oral antibiotics (co-trimoxazole, doxycycline, moxifloxacin or rifabutin) guided by participant susceptibility and tolerance. Oral moxifloxacin 10-15mg/kg once daily, maximum dose 400mg

DRUGBedaquiline

Adult: during consolidation in combination with one to three oral antibiotics (co-trimoxazole, doxycycline, moxifloxacin, bedaquiline or rifabutin) guided by participant susceptibility and tolerance. Oral bedaquiline (18-64 years of age) 400mg once daily for the first two weeks followed by 400mg thrice weekly for 22 weeks (maximum duration of 6 months).

DRUGRifabutin

Adult: during consolidation in combination with one to three oral antibiotics (co-trimoxazole, doxycycline, moxifloxacin, bedaquiline or rifabutin) guided by participant susceptibility and tolerance. Oral rifabutin: 5mg/kg once daily, maximum 300-450mg. Children: During consolidation in combination with one to three oral antibiotics (co-trimoxazole, doxycycline, moxifloxacin or rifabutin) guided by participant susceptibility and tolerance. Oral rifabutin 5mg/kg once daily

Locations(50)

St George Hospital

Kogarah, New South Wales, Australia

Queensland Children's Hospital

South Brisbane, Queensland, Australia

Princess Alexandra Hospital

Woolloongabba, Queensland, Australia

Austin Hospital

Heidelberg, Victoria, Australia

Royal Melbourne Hospital

Parkville, Victoria, Australia

Royal Perth Hospital

Perth, Western Australia, Australia

Royal Adelaide Hospital

Adelaide, Australia

Sunshine Coast University Hospital

Birtinya, Australia

Royal Prince Alfred Hospital

Camperdown, Australia

The Prince Charles Hospital

Chermside, Australia

Gold Coast University Hospital

Gold Coast, Australia

Greenslopes Private Hospital,

Greenslopes, Australia

Sir Charles Gairdiner Hospital

Nedlands, Australia

John Hunter Hospital

New Lambton, Australia

John Hunter Children's Hospital

New Lambton Heights, Australia

Perth Children's Hospital

Perth, Australia

The Alfred

Prahran, Australia

Sydney Children's Hospital

Randwick, Australia

Mater Adult Hospital

South Brisbane, Australia

Macquarie University Hospital

Sydney, Australia

The Children's Hospital at Westmead

Westmead, Australia

Westmead Hospital

Westmead, Australia

Rigshospitalet

Copenhagen, Denmark

Soroka Medical Centre

Beer-Sheeva, Israel

Carmel Medical Centre

Haifa, Israel

Rambam Health Care Campus

Haifa, Israel

Hadassah Ein Kerem Hospital

Jerusalem, Israel

Schneider

Petah Tikva, Israel

Sheba Medical Centre

Ramat Gan Tel Aviv, Israel

Erasmus MC Sophia Children's Hospital

Rotterdam, Netherlands

Tan Tock Seng Hospital Pte Ltd

Singapore, Singapore

Kaohsiung Medical University Hospital

Kaohsiung City, Taiwan

National Taiwan University Hospital

Taipei, Taiwan

Belfast City Hospital

Belfast, United Kingdom

Birmingham Children's Hospital

Birmingham, United Kingdom

Birmingham Heartlands Hospital

Birmingham, United Kingdom

Bristol Royal Hospital for Children

Bristol, United Kingdom

Noah's Ark Childrens Hospital for Wales

Cardiff, United Kingdom

Royal Hospital for Children and Young People, Edinburgh

Edinburgh, United Kingdom

Western General Hospital

Edinburgh, United Kingdom

Queen Elizabeth University Hospital, Glasgow

Glasgow, United Kingdom

Alder Hey Children NHS Foundation Trust

Liverpool, United Kingdom

Royal Brompton Hosptial

London, United Kingdom

Royal Manchester Children's Hospital

Manchester, United Kingdom

Nottingham Children's Hosptial

Nottingham, United Kingdom

Queens Medical Centre

Nottingham, United Kingdom

Welcome Wolfson Adult CF Centre (City Hospital Campus)

Nottingham, United Kingdom

University Hospital Llandough

Penarth, United Kingdom

Southampton General Hospital

Southampton, United Kingdom

Wythenshawe Hospital

Wythenshawe, United Kingdom

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NCT04310930