MedPath

BACE Trial Substudy 2 - FarmEc Substudy

Phase 3
Completed
Conditions
Chronic Obstructive Pulmonary Disease
Interventions
Drug: Placebo
Registration Number
NCT02205255
Lead Sponsor
Wim Janssens
Brief Summary

A second sub-analysis of the BACE trial will include a detailed cost-effectiveness study.

Detailed Description

Our multicenter randomized trial executed in one country will provide an excellent tool for more precise health economic assessments. In a first approach, rough estimates on savings of direct costs in the entire study cohort will be made by taking into account the Flemish average costs for a single hospitalization day at a respiratory ward, for a day at intensive care, for an emergency visit, for a home physician contact and for an antibiotic-steroid course. A more detailed cost-effectiveness and cost-utility analysis at 3 and 9 months interval will only be performed in case significant clinical benefits are found in favor of the active treatment.

For this purpose medical resource use data will be collected retrospectively via hospital invoices (direct costs including drugs, physician visits, laboratory tests, technical exams, medical imaging, hospital stay) but also prospectively via patient diaries, to cover direct and indirect costs during the entire outpatient period, and will be linked to EQ5D scores.

Patient will have to give informed consent that additional to the clinical evaluation, invoices will be collected. However, individual patients can still opt out for these analyses (sub-study) and only participate in the medical intervention study (main study).

Recruitment & Eligibility

Status
COMPLETED
Sex
All
Target Recruitment
350
Inclusion Criteria
  • Established diagnosis of COPD by medical doctor (based on clinical history OR pulmonary function test)
  • Smoking history of at least 10 pack-years (10 pack-years are defined as 20 cigarettes a day for 10 years, or 10 cigarettes a day for 20 years, etc.)
  • Current hospitalization for potential infectious AECOPD treated with standard therapy
  • History of at least one exacerbation during the last year (prior to the current hospital admission) for which systemic steroids and/or antibiotics were taken
  • ECG at admission
Exclusion Criteria
  • Mechanical or non-invasive ventilation at moment of randomization (D1)
  • Long QT interval on ECG (QTc > 450msec for males or > 470msec for females)
  • History of life-threatening arrhythmias
  • Myocardial infarction (NSTEMI or STEMI) less than 6 weeks before start of study drug
  • Unstable angina pectoris or acute myocardial infarction (NSTEMI or STEMI) at admission
  • Drugs with high risk for long QT interval and torsade de pointes (amiodarone, flecainide, procainamide, sotalol, droperidol, haldol, citalopram, other macrolides)
  • Documented uncorrected severe hypokalemia (K+ < 3.0 mmol/L) or hypomagnesemia (Mg2+ < 0.5 mmol/L)
  • Chronic systemic steroids (> 4 mg methylprednisolone /day for β‰₯ 2 months)
  • Actual use of macrolides for at least 2 weeks
  • Allergy to macrolides
  • Active cancer treatment
  • Life expectancy < 3 months
  • Pregnant or breast-feeding subjects. Woman of childbearing potential must have a pregnancy test performed and a negative result must be documented before start of treatment

Study & Design

Study Type
INTERVENTIONAL
Study Design
PARALLEL
Arm && Interventions
GroupInterventionDescription
PlaceboPlaceboN = 250 From day 1 up to and including day 3: 500 mg placebo PO once a day From day 4 up to and including day 90: 250 mg placebo PO once every 2 days
AzithromycinAzithromycinN = 250 From day 1 up to and including day 3: 500 mg azithromycin PO once a day From day 4 up to and including day 90: 250 mg azithromycin PO once every 2 days
Primary Outcome Measures
NameTimeMethod
Total cost (direct and Indirect cost) during the entire study participationAt 3 month interval

Direct costs (including drugs, physician visits, laboratory tests, technical exams, medical imaging, hospital stay) will be assessed by collecting the medical resource use data retrospectively via hospital invoices and prospectively via patient diaries.

Indirect costs (relating to time, convenience, and transportation) will be assessed by collecting the medical resource use data prospectively via patient diaries.

This outcome measure will also be analysed in following subgroups:

* Male vs female

* Smoker vs ex-smoker (stopped smoking \> 6 months)

* GOLD A, B vs GOLD C vs GOLD D

* Former GOLD I, II vs III vs IV

* High CRP (\> 50 mg/dL) vs low CRP (\< 50 mg/dL)

* Age \< 60 years vs age 60 - 70 years vs age \> 70 years

* Anthonissen I vs Anthonissen II vs Anthonissen III at admission

* ICS use vs no ICS use

Secondary Outcome Measures
NameTimeMethod
Total cost (direct and Indirect cost) during the entire study participationAt 9 month interval

Direct costs (including drugs, physician visits, laboratory tests, technical exams, medical imaging, hospital stay) will be assessed by collecting the medical resource use data retrospectively via hospital invoices and prospectively via patient diaries.

Indirect costs (relating to time, convenience, and transportation) will be assessed by collecting the medical resource use data prospectively via patient diaries.

This outcome measure will also be analysed in following subgroups:

* Male vs female

* Smoker vs ex-smoker (stopped smoking \> 6 months)

* GOLD A, B vs GOLD C vs GOLD D

* Former GOLD I, II vs III vs IV

* High CRP (\> 50 mg/dL) vs low CRP (\< 50 mg/dL)

* Age \< 60 years vs age 60 - 70 years vs age \> 70 years

* Anthonissen I vs Anthonissen II vs Anthonissen III at admission

* ICS use vs no ICS use

Trial Locations

Locations (20)

UZ Brussel

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Brussel, Brussel Hoofdstedelijk Gewest, Belgium

Jessa Ziekenhuis

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Hasselt, Vlaanderen, Belgium

AZ Groeninge Ziekenhuis

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Kortrijk, Vlaanderen, Belgium

Heilig Hart Ziekenhuis

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Roeselare, Vlaanderen, Belgium

UZ Gent

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Gent, Vlaanderen, Belgium

CHU Charleroi

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Charleroi, WalloniΓ«, Belgium

Onze-Lieve-Vrouwziekenhuis

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Aalst, Belgium

CHU Liège

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Liège, Wallonië, Belgium

St. Pieterziekenhuis

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Brussel, Brussels Hoofdstedelijk Gewest, Belgium

ZNA Middelheim

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Antwerpen, Vlaanderen, Belgium

St. Jan Brugge Ziekenhuis

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Brugge, Vlaanderen, Belgium

UZ Gasthuisberg

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Leuven, Vlaanderen, Belgium

Clinique Sainte-Elisabeth

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Namur, Belgium

St. Augustinus Ziekenhuis

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Antwerpen, Vlaanderen, Belgium

Imelda Ziekenhuis

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Bonheiden, Vlaanderen, Belgium

Maria Middelaresziekenhuis

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Gent, Vlaanderen, Belgium

St. Andriesziekenhuis

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Tielt, Vlaanderen, Belgium

CHU Mont-Godinne

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Yvoir, WalloniΓ«, Belgium

Grand HΓ΄pital de Charleroi

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Gilly, WalloniΓ«, Belgium

Clinique Reine Astrid

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Malmedy, Belgium

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