Overview

Childhood Asthma Research and Education (CARE) Network Trial - Montelukast or Azithromycin for Reduction of Inhaled Corticosteroids in Childhood Asthma (MARS)

Status:
Terminated

Trial end date:
2007-03-01

Target enrollment:
0

Participant gender:
All

Summary

The MARS trial is a randomized, double-blind, parallel group study that compares the capacity of azithromycin or montelukast to placebo as effective adjunctive therapy that allows reduction of inhaled corticosteroids in children ages 6 to 17 years with moderate to severe persistent asthma. The primary null hypothesis is that in children with moderate-to-severe persistent asthma, a macrolide antibiotic (azithromycin) or a leukotriene receptor antagonist (montelukast) will provide a steroid-sparing effect when compared to placebo as the dose of inhaled corticosteroid is reduced. This will be tested following achievement of control of symptoms with moderate to high-dose inhaled corticosteroid in combination with a long-acting bronchodilator agonist. Use of these doses for the inhaled corticosteroid will be based on NHLBI step-up guidelines to achieve asthma control.

Phase:

Phase 4

Accepts Healthy Volunteers?

Details

Lead Sponsor:

National Heart, Lung, and Blood Institute (NHLBI)

Treatments:

Azithromycin
Budesonide
Montelukast
Salmeterol Xinafoate

Criteria

Inclusion Criteria:

At Enrollment (V0):

- Age 6-17 years at time of enrollment. A goal of 33% minority and 40% female subjects
will be incorporated in recruitment

- Weighs at least 25 kg

- Asthma diagnosed by a physician and present for at least one year prior to study entry

- Moderate to severe persistent asthma:

1. Patients will be identified in the following general categories. The general
principle is that patients will be uncontrolled on a relatively low dose of ICS
that can be stepped-up, or controlled on a moderate or high dose of ICS that can
be stepped-down.

i) On low dose ICS with or without salmeterol and uncontrolled. This patient will
be treated with budesonide and salmeterol to determine eligibility criteria. If
the addition of salmeterol results in control of symptoms, the patient would be
excluded from MARS. If control was not established on low dose budesonide and
salmeterol, the dose of budesonide would be increased and entry criteria
evaluated based on the algorithm in Figure 1.

ii) On a dose of ICS equivalent to budesonide at 400 mcg per day with or without
any other medication and uncontrolled. This patient will be treated with
budesonide and salmeterol to determine eligibility criteria.

iii) On a dose of ICS equivalent to budesonide at 800 mcg per day with or without
any other medication and controlled.

iv) On a dose of ICS equivalent to budesonide at 1600 mcg per day with or without
any other medication and uncontrolled but not requiring prednisone acutely. These
patients will be followed to see if they become well controlled with increased
adherence or more careful monitoring of symptoms.

2. Examples are given for Advair as this drug is a commonly used form of ICS and
LABA:

i) Patients on Advair 100/50 bid and inadequately controlled ii) Patients on
Advair 250/50 bid and inadequately controlled iii) Patients on Advair 250/50 bid
and well controlled for greater than 3 months and being considered for
stepping-down to Advair 100/50 iv) Patients well controlled on Advair 100/50 bid
+ either montelukast or theophylline for greater than 3 months and being
considered for stepping-down to Advair 100/50 bid alone v) Patients on Advair
500/50 bid and well controlled for greater than 3 months and being considered for
stepping-down to Advair 250/50 vi) Patients well controlled on Advair 250/50 bid
+ either montelukast or theophylline for greater than 3 months and being
considered for stepping-down to Advair 250/50 bid alone

3. Patients on an equivalent of budesonide 400 mcg, 800 mcg, or 1600 mcg per day
with no symptoms, but with an FEV1 less than 80% predicted, will be enrolled as
uncontrolled and observed closely for symptoms or low peak flows for 2 weeks. The
rationale for enrolling these patients and observing them as "uncontrolled" is
that patients with an FEV1 below the range of normal may be having symptoms
and/or low peak flows that will become apparent under close observation after
appropriate education. Note that a percent predicted value for FEV1 will be used
only at the enrollment visit, with criteria for control and inadequate control
during both run-in and during the double-blind portions of the study using the
highest FEV1 value obtained during run-in for decisions prior to randomization
and the FEV1 at randomization for decisions subsequent to that visit.

- FEV1 at least 80% predicted if there is going to be step-down at enrollment or at
least 50% predicted if already suboptimally controlled historically and to be observed
for 2 weeks to define baseline symptoms. FEV1 measurements will be obtained
pre-bronchodilator.

- Demonstrate a bronchodilator response with an improvement in FEV1 of at least 12% or
airway responsiveness to methacholine with a PC20 less than 12.5 mg/ml.

1. Bronchodilator responsiveness testing will be done at Visit 0 (Enrollment) in all
patients using 4 puffs albuterol.

2. Methacholine challenge will be done at Visit 1 (Step-up) in patients who did not
respond to bronchodilator at Visit 0. Patients with a FEV1 less than 70%
predicted or an upper respiratory infection at the time of Visit 1 will have a
second bronchodilator challenge rather than a methacholine.

- Varicella immunization complete (unless the subject has already had clinical
varicella). If the subject needs varicella vaccine, this will be arranged with the
primary care physician and must be received prior randomization

- Willingness to provide informed consent by the child's parent or guardian

- Nonsmoker in the past year; in addition, no use of smokeless tobacco products in the
year prior to study entry

Exclusion Criteria:

At Enrollment (V0):

- More than four courses of systemic corticosteroids for asthma during the 12 months
prior to study entry

- More than one hospitalization for wheezing illnesses within the 12 months prior to
study entry

- Current treatment with antibiotics for diagnosed sinus disease

- History of severe sinusitis requiring sinus surgery within the past 12 months

- Use of maintenance oral or systemic antibiotics for treatment of an ongoing condition

- Use of macrolide antibiotics within the 6 weeks prior to study entry

- Requirement for prednisone therapy for concurrent illness, e.g., RA, SLE, IBD

- Asthma exacerbation requiring systemic corticosteroids within 4 weeks of study entry

- Contraindication for use of macrolide or LTRA

- Presence of lung disease other than asthma, such as cystic fibrosis and
bronchopulmonary dysplasia. Evaluation during the screening process will assure that
an adequate evaluation of other lung diseases has been performed

- Presence of other significant medical illnesses (cardiac, liver, gastrointestinal,
endocrine, any seizure disorder except febrile seizure in infancy) that would place
the study subject at increased risk of participating in the study

- Use of digoxin, ergotamine or dihydroergotamine, triazolam, carbamazepine,
cyclosporine, hexobarbital, and phenytoin, and similar classes of medication will be
specifically excluded

- Use of omalizumab within one year of study entry

- Gastroesophageal reflux symptoms not controlled by standard medical therapy

- Immunodeficiency disorders

- History of respiratory failure requiring mechanical ventilation for asthma within 5
years

- History of hypoxic seizure due to asthma

- Inability of the child to ingest the study drug

- Participation presently or in the past month in another investigational drug trial

- Evidence that the family may be unreliable or nonadherent, or may move from the
clinical center area before trial completion

- Pregnant or breastfeeding

- Receiving hyposensitization therapy other than an established maintenance (continuous
for 3 months duration or longer) regimen

At Randomization (V2):

- Still uncontrolled on step-up dosing of 1600 mcg budesonide + salmeterol BID

- Abnormal liver enzyme laboratory test results

- Abnormal QTc interval or evidence of a rhythm abnormality

- Failure to complete diary cards at expected levels (at least 75% of days) during the
observation period

- Failure to adhere with oral medication use at least 80% during run-in

- Need for oral corticosteroids for a reason other than Step Up during run-in period