Asthma Clinical Trial
Official title:
Childhood Asthma Research and Education (CARE) Network Trial - Montelukast or Azithromycin for Reduction of Inhaled Corticosteroids in Childhood Asthma (MARS)
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.
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 (Mac - azithromycin) or a
leukotriene receptor antagonist (LTRA - montelukast) will provide a steroid-sparing effect
when compared to placebo as the dose of inhaled corticosteroids (ICS - budesonide) is
reduced. This will be tested following achievement of control of symptoms with moderate to
high-dose ICS in combination with a long-acting bronchodilator agonist (LABA - salmeterol).
Use of these doses for the inhaled corticosteroid will be based on NHLBI step-up guidelines
to achieve asthma control. Inadequate asthma control is defined as either:
1. chronic poor control: a) symptoms, or albuterol use for symptoms or low peak flow, or
peak flow less than 80% baseline on greater than 3 days per week on average, or b)
nocturnal awakenings for asthma symptoms requiring albuterol 2 or more nights over 2
weeks of observation, or c) FEV1 less than 80% of the best pre-randomization value on 2
consecutive visits 1-4 days apart, or
2. an asthma exacerbation as determined by need for systemic corticosteroids
Treatment in the run-in period will be determined by the child's status at the first visit.
At enrollment (V0) all patients will be given budesonide as the ICS and salmeterol as the
LABA. Children will be treated with salmeterol BID and a dose of ICS based on chronic
medication use with stepping-down based on time and symptoms until criteria for inadequate
control as indication for stepping-up the dose of ICS. When inadequate control is documented
(V1), a four-day course of prednisone will be administered and the dose of ICS (still
administered with salmeterol BID) will be doubled to establish control. The children will be
followed with monthly clinic visits and interim phone calls, emphasizing use of daily diary
to document symptoms and doses of albuterol required. Reestablishment of control during a
2-week interval will prompt randomization. If control is not yet established by the first
increase in ICS dose during the stabilization period, the dose can be doubled along with a
second prednisone course until a maximum of budesonide of 1600 mcg/day is attained. The
daily dose of budesonide at randomization will be a minimum of 800 mcg to allow for a
maximum of 4-fold reduction of dose, and a maximum of 1600 mcg to allow for patient safety
considering side effects of high dose ICS.
When clinical control is achieved by the increased dose of ICS, a child will then be
randomized (V2) to one of the three treatment arms, (1) placebo (one placebo tablet and one
or two placebo capsules), (2) azithromycin (one placebo tablet and one or two capsules
containing azithromycin with the dose based on weight), or (3) montelukast (one tablet
containing montelukast with the dose based on age as indicated in the package insert and one
or two placebo capsule). Children will be followed for an additional six weeks on the dose
of ICS that achieved control ("1X") + salmeterol BID with the study medication (V3). They
will then undergo three 6-week periods of ICS reduction (V4, V5, V6), first to ¾ of the
control dose ("0.75X"), then ½ of the control dose ("0.5X") and then ¼ of the control dose
("0.25X"), each using salmeterol BID as concomitant medication. The ICS dosing and
salmeterol will be open-label. Criteria for treatment failure and discharge from the study
will be an established set of criteria that indicate reappearance of inadequate control of
asthma or an exacerbation of asthma.
At the end of the double-blind administration of oral study medication (V6), patients not
discharged from the study because of having met one of the criteria for inadequate control
of asthma will have their study medication discontinued, with subjects continuing to take
placebo capsules in addition to ¼ ICS plus salmeterol. They will then be followed for an
additional 6-week single-blind wash-out period with an interim contact by phone at 3 weeks
to determine the course of asthma control to determine the persistence of effect off of the
study medication (V7).
The procedures to be performed at V0 are informed consent, pregnancy test, complete physical
exam, spirometry, and bronchodilator response. The procedures to be performed at V1 are
spirometry, complete blood count, blood IgE and eosinophils, brief physical exam, EKG, and
genotyping. The following procedures will be performed at each of V2 through V7: brief
physical exam, spirometry, forced oscillometry, exhaled nitric oxide, asthma control
questionnaire, asthma-specific quality-of-life questionnaire, and sinusitis questionnaire.
In addition, allergy skin testing will be performed at V2, pregnancy tests at V2 through V6,
methacholine challenge at V2 and V3, and polymerase chain reaction for atypical organisms
and macrolide antibiotic resistance (nasal wash) at V2, V5, and V7.
Finally, children will maintain daily diary records of morning and evening symptoms, peak
expiratory flow rates, and rescue medication use.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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