Asthma Clinical Trial
Official title:
Asthma Clinical Research Network (ACRN)
This study will establish a network of interactive asthma clinical research groups to evaluate current therapies, new therapies, and management strategies for adult asthma.
BACKGROUND:
Asthma is an increasingly serious cause of morbidity and mortality in the United States.
There are approximately 12 million asthmatics, and the disease affects both sexes and
impacts all racial and ethnic groups. It is now recognized that asthma is a complex disease
of varied etiology, which is triggered by a number of factors (e.g., allergens, drugs,
chemicals, exercise, cold air, infections, and emotions), making asthma therapy difficult
and sometimes complicated. Multiple drugs, including medications to treat and control
symptoms (bronchodilator agents such as beta-adrenergic agonists, theophylline, and
anticholinergics) and medications thought to control underlying airway inflammation (e.g.,
inhaled and systemic corticosteroids, cromolyn sodium, and nedocromil), are often required.
Despite major advances in the understanding of the etiology and pathophysiology of asthma
and the development of new therapeutic modalities, the prevalence, severity, and mortality
from asthma in all age groups have increased over the past decade. Mortality rates are
disproportionately high in urban and rural minority populations. Hospitalizations for asthma
have doubled in adults and increased five-fold for children over the past 20 years. Asthma
continues to place a heavy burden on patients and their families, the health care system,
and society as a whole. Therefore, new approaches are needed to help alleviate this growing
problem.
A particularly important need at this juncture is a mechanism for the rapid evaluation of
new and existing therapeutic approaches for asthma and for the dissemination of laboratory
and clinical findings to the health care community. The Asthma Clinical Research Network
(ACRN) program seeks to accomplish this through the development of a network of interactive
asthma clinical groups that conduct clinical studies employing common protocols in a
coordinated and multidisciplinary setting. This will ensure ready access to an adequate
number of well characterized patients from diverse populations and age groups. It will also
bring together and coordinate the necessary clinical expertise and administrative resources
to conduct multiple therapeutic studies. Centralized protocols will promote high quality
design, decrease the variability in supportive modalities, and reduce the redundant
utilization of resources required for rapidly conducting multiple independent clinical
studies. The separate data coordinating center supports protocol and questionnaire
development, sample size calculations, complete data analysis, and overall study
coordination.
The initiative was developed by the Pulmonary Diseases Advisory Committee working group,
approved by the full committee at the February 1992 meeting, and given concept clearance by
the National Heart, Lung, and Blood Institute (NHLBI) Advisory Council in May 1992.
DESIGN NARRATIVE:
The Beta-Agonist (Bags) study compared the safety and efficacy of regular plus "as needed"
use of inhaled albuterol to the "as needed" use of inhaled albuterol in 255 patients with
asthma of mild severity. A total of 230 patients completed the study. The study was
randomized, double-blind, and placebo-controlled with parallel groups. Following a 6-week
single-blind run-in period, patients were randomized in a double-blind manner and treated
for 16 weeks. There was a 4-week withdrawal, or run-out, period. Changes in lung function
and asthma symptoms were assessed to determine whether regular or "as needed" beta-agonist
use was more beneficial in the treatment of mild asthma. Specific outcome measures included
morning (AM) PEF, airway responsiveness, spirometric values, evening (PM) to AM PEF
difference index, asthma symptoms, quality of life measures, use of rescue medications, and
episodes of adverse asthma control. Recruitment began in December 1994. The study has
completed and results have been published.
The Colchicine in Moderate Asthma (CIMA) study examined if colchicine offered therapeutic
benefit in the management of 71 patients with moderate asthma when corticosteroids were
discontinued. The study was randomized, double-blind, and placebo-controlled with two
parallel groups. A 2-week run-in with inhaled corticosteroid was followed by 2 weeks with
inhaled corticosteroid and colchicine or placebo, and then by 6 weeks with no inhaled
corticosteroid but with colchicine or placebo. There was a 6-week single-blind run-out.
Outcome measures included treatment failure after cessation of inhaled corticosteroid, FEV1
change, PM to AM PEF difference index, airway responsiveness, asthma symptoms, quality of
life measures, use of rescue medications, and episodes of adverse asthma control. The
protocol was approved in April 1994. Recruitment ran from February 1996 through August 1996.
Results have been published.
The Salmeterol or Corticosteroids (SOCS) study was a randomized, double-blind study to
determine the utility of treating patients with moderately severe asthma with long-acting
beta-agonists in place of inhaled corticosteroids (ICS). A total of 164 patients were
randomized into one of the following three treatment arms (double-blind and double-dummy):
1) placebo; 2) inhaled corticosteroid triamcinolone alone; or 3) beta-agonist salmeterol
alone. Treatment continued for 16 weeks, followed by a 6-week run-out period in which all
patients were placed on placebo. The purpose of the run-out period was to evaluate the
effects of treatment cessation on asthma control. To compare efficacy of therapy, the
primary outcome variable was the change in AM PEF from the final week of the run-in period
to the final week of the double-blind treatment period. To compare duration benefit, the
primary outcome variable was again AM PEF, with a comparison of the change from the final
week of the run-in period to the second and final weeks of the run-out period. Secondary
endpoints included other markers of asthma severity (e.g., FEV1, symptom diaries,
beta-agonist rescue, quality-of-life scores, methacholine responsiveness, and asthma
exacerbations). To evaluate markers of inflammation, sputum induction was performed on all
patients, and bronchoalveolar lavage and bronchial biopsy were performed on a subset of
patients. Enrollment began in February 1997 and ended in July 1998. Results have been
published.
The Salmeterol± Corticosteroids (SLIC) study examined the addition of a long acting
beta-agonist, salmeterol, on a scheduled basis for patients with moderate asthma whose
symptoms were sub-optimally controlled by using an inhaled beta-agonist on an "as needed"
basis and an inhaled corticosteroid on a scheduled basis. The study determined if the
addition of salmeterol on a scheduled basis permitted a reduction in dose, and/or
elimination of inhaled corticosteroids over time, without a concomitant increase in
asthmatic symptoms or a decrease in the bronchoprotective effect to aerosolized
methacholine. Recruitment of randomized patients with moderate asthma began in January 1997.
Additional patients were randomized at the Harlem Center, a center added to the network in
December 1995. The enrollment of 175 patients ended in July 1998 and the last patient visits
were completed in January 1999. Results have been published.
The Dose of Inhaled Corticosteroids with Equisystemic Effects (DICE) study estimated
dose-response curves with respect to adrenal suppression for six distinct inhaled
corticosteroids. The inhaled steroids and delivery systems were characterized in terms of
systemic effects so that doses that produced "equi-systemic" effects could be subsequently
compared in future efficacy studies, including the efficacy study "Measuring Inhaled
Corticosteroid Efficacy" (MICE). In DICE, a total of 156 (58% male and 31% minority)
patients with mild to moderate asthma had a baseline visit and a placebo run-in period to
practice taking scheduled doses (4 puffs twice a day) from a metered dose inhaler for 1
week. At the second visit, patients were randomized to placebo or to one of the following
six steroid arms, including: 1) beclomethasone dipropionate metered dose inhaler (MDI); 2)
budesonide dry powder; 3) flunisolide MDI; 4) fluticasone propionate MDI; 5) fluticasone
propionate dry powder; or 6) triamcinolone acetonide MDI. The study addressed the following
questions: 1) Were there dose-response relationships in the suppression of overnight plasma
cortisol with the various inhaled corticosteroids and delivery systems?; 2) If the
dose-response relationships existed, at which doses were comparable systemic effects evident
as determined by suppression of overnight plasma cortisol?; and 3) If dose-response
relationships existed, which dose produced a 10%, 20%, 30%, or 40% suppression of adrenal
steroid secretion (cortisol) for each inhaled steroid and delivery system? DICE was
initiated in September 1998 and completed in November 1999. Results have been published.
The Measuring Inhaled Corticosteroid Efficacy (MICE) pilot study was approved by the
Protocol Review Committee in August 1998. MICE used doses of inhaled corticosteroid for the
full MICE protocol as derived from DICE, which induced minimal cortisol suppression (highest
deliverable dose that caused less than 5% cortisol suppression), 20% to 30% cortisol
suppression, and 40% to 60% cortisol suppression. The intent was to determine if different
inhaled corticosteroids, which had equisystemic effects, had differential salutary
therapeutic effects in chronic asthma, or if therapeutic efficacy paralleled systemic
effects. MICE was a 24-week, randomized, open-label, prospective, multi-center study
examining the effect of inhaled beclomethasone dipropionate (BDP) and fluticasone propionate
(FP) both with an Opti-Chamber spacer device. The inhaled corticosteroids were administered
to 30 patients in doses of increasing systemic effect to examine the corresponding effects
on pulmonary function, bronchial hyper-responsiveness, asthma control, and resolution of
airway inflammation in patients with persistent asthma. The intent was to compare the
estimates of systemic effect for BDP and FP, derived from the DICE pilot study in which BDP
and FP were administered in 1-week intervals, to that which occurred when BDP and FP doses
were administered over 3- to 6-six week intervals with incremental doses. MICE also explored
which efficacy/systemic relationships, if any, suggested that there may be a difference
between the two prototype inhaled corticosteroids, BDP and FP. Recruitment was completed in
the spring of 2000. Results have been published.
The Beta Agonist Response by Genotype (BARGE) study was reviewed by the Protocol Review
Committee in December 1998. Recruitment started in September 1999. BARGE was a 54-week
randomized, double-blind, crossover study comparing the effects of regularly scheduled use
of inhaled albuterol (2 puffs four times a day) to placebo. Two groups of 36 participants
each included individuals who had mild to moderate asthma and who differed by their genotype
at the codon for the 16th amino acid of the B2-adrenergic receptor. A total of 36
participants harbored the B16-Arg/Arg genotype and the other 36 harbored the B16-Gly/Gly
genotype at the B2-adrenergic receptor. Qualified participants entered a 6-week single-blind
run-in period during which they were treated with an inhaled placebo (2 puffs 4 times a day)
and given inhaled ipratropium bromide for use as a rescue medication. Asthma control was
characterized by AM PEF, spirometric values, AM/PM PEF variability index, asthma symptoms,
quality of life, use of rescue medications, and occurrence of events of adverse asthma
control. Baseline data were obtained on airway responsiveness, the protective effect of
albuterol against methacholine-induced bronchoconstriction, the maximum bronchodilator
effect of albuterol, and exhaled nitric oxide. Participants were then randomized to a
16-week double-blind treatment phase in which they received either inhaled albuterol or
placebo (two puffs 4 times a day). Asthma control was monitored by the above indicators
during this time. At the end of the blinded treatment period, all participants were returned
to single-blind regular use of a placebo inhaler (2 puffs 4 times a day) for an 8-week
run-out period. Following cross-over to double-blinded treatment with albuterol or placebo,
the 8-week run-out period also served as the run-in period for the second stage of the
study. Asthma control was monitored by the same indicators as in the first stage. At the end
of the second blinded treatment period, all participants were returned to single-blind
regular use of a placebo inhaler (2 puffs 4 times a day) for an 8-week run-out period.
During the entire study, participants used inhaled ipratropium bromide as rescue medication
to avoid the confounding effects of B2-adrenergic stimulation on the outcome variables to be
monitored. In the event that an episode of adverse asthma control responded incompletely to
ipratropium, albuterol was used as a superseding rescue medication. Comparisons of asthma
control, within each genotypic group during periods of randomized treatment, were assessed
as the difference in the change in outcome variables between the end of Stage 1 randomized
treatment and the end of Stage 1 run-in, and between the end of Stage 2 randomized treatment
and the end of Stage 1 run-out. The study was completed and results have been published.
The Improving Asthma Control Trial (IMPACT) was a double-blind, randomized, parallel group
design clinical study to determine the best long-term strategy for treating adults with mild
asthma who experienced symptoms more than occasionally. The study tested whether these
patients should be taking anti-inflammatory medications on a daily basis and whether a newer
class of medications provided the same benefit as older drugs. In the IMPACT study, 225
adults with mild asthma, who had more than occasional symptoms, were enrolled in six
clinical research centers. Following an initial evaluation, patients were randomized to
receive either a twice daily inhaled corticosteroid, a twice daily anti-leukotriene, or a
placebo. All patients received treatment for symptoms if, and when, they occured. The
primary outcome was AM PEF. Other outcomes included FEV1 before and after bronchodilator
treatment, the frequency of exacerbations, the degree of asthma control, the number of
symptom-free days, and the quality of life. Recruitment ended in 2003. Study results were
published in the April 14, 2005 issue of the New England Journal of Medicine. In April 2001
NHLBI initiated an ancillary study to IMPACT entitled "Modification of Allergic Immunologic
Response by Leukotriene Antagonists" under R01HL67684. The ancillary study has its own site
in this database.
The Smoking Modulates Outcomes of Glucocorticoid Therapy in Asthma (SMOG) study was a
randomized, double-blind, cross-over study, which compared the effect of inhaled
corticosteroid treatment delivered twice daily for 8 weeks in the following two groups of
patients with persistent asthma: 1) smokers; and 2) non-smokers. Smokers and non-smokers
were matched into pairs according to gender and FEV1 status prior to the run-in period. Each
member of the matched pair was randomized together to the same crossover sequence. There
were 96 patients ages 18 to 35. The primary outcome was change in pre-bronchodilator FEV1
over the 8-week treatment period in smokers compared with non-smokers. Secondary outcomes
were AM and PM PEF, PC20 methacholine, and markers of inflammation in induced sputum. A
secondary comparison examined the effect of 8 weeks of treatment with a leukotriene receptor
antagonist in asthmatics who smoked to those who did not. An additional analysis compared
the response to inhaled corticosteroid with the response to leukotriene receptor antagonist.
The study was completed and results have been submitted to a journal for publication.
The Salmeterol and Leukotriene Modifiers versus ICS Treatment (SLIMSIT) study initiated
recruitment in September 2002. The goal was to randomize 180 participants. SLIMSIT was a
36-week, double-blind, placebo-controlled, cross-over study, with time to treatment failure
as the primary endpoint. Prior to each double-blind treatment phase, participants underwent
a 4-week run-in period with combined inhaled beclomethasone HFA and the leukotriene receptor
antagonist (LTRA) montelukast. This was followed by 14 weeks of double-blind treatment.
During the initial 4-week run-in period, participants who met National Asthma Education
Program criteria for moderate persistent asthma received a controller regimen to obtain
baseline information on symptoms, beta-agonist use, and PEF for use in defining treatment
failure for each participant over the duration of the study. The final visit of this run-in
period served as the baseline of comparison for the study variables measured during the
initial treatment phase. At the end of the initial run-in, participants with stable asthma
symptoms were randomized to one of the following two treatment regimens for 14 weeks: 1)
daily oral placebo, twice daily inhalation of salmeterol 50 mg by dry powder inhaler (DPI),
and twice daily inhalation of beclomethasone HFA 80 mg by MDI; or 2) once daily oral
montelukast 10 mg, twice daily inhalation of salmeterol 50 mg by DPI, and twice daily
inhalation of placebo. Active beclomethasone HFA and the beclomethasone HFA placebo were
given via a MDI delivery device, while salmeterol was given by a DPI Diskusâ. A computer
interface randomized participants into the two treatment groups, stratifying by clinical
center and FEV1 at the randomization visit (less than 80% versus greater than 80% of
predicted FEV1). During the first treatment period, participants made three visits to the
clinic over 14 weeks. These visits included re-assessment of the study variables and careful
monitoring for increasing asthma symptoms and potential treatment failure. Subsequently,
participants entered a second run-in period in which they received single-blind treatment
with inhaled beclomethasone HFA and oral montelukast as in the first run-in period. At the
end of the second run-in period, participants crossed over to the alternate treatment
regimen for the second 14-week treatment phase, which included three visits to the clinic.
These visits again included re-assessment of the study variables and careful monitoring for
increasing asthma symptoms and potential treatment failure. DSMB recommended termination of
the study prior to target enrollment because sufficient data about the primary outcome had
been obtained. SLIMSIT results were presented at the May 2005 American Thoracic Society
Annual Meeting. The data are under analysis for subsequent publication.
The Predicting Responses for Inhaled Corticosteroid Efficacy (PRICE) study was a follow-up
study that looked for additional predictive biomarkers of response to inhaled
corticosteroids. The study also evaluated whether short-term response to inhaled
corticosteroids predicted asthma control and exacerbation rate, and whether it correlated
with elastic recoil and upstream resistance. In this study, adults with a history of asthma
underwent 6 weeks of ICS treatment, then were stratified by response and randomized in a
double-blind fashion to continue ICS therapy or receive placebo for 16 weeks. ACRN
investigators found that after 6 weeks of ICS therapy, patients with a good (15%) versus
poor (less than 5%) increase in FEV1 experienced significantly better asthma control during
continued ICS treatment. Interestingly, nitric oxide concentration in exhaled breath and
airway sputum eosinophils, generally considered biomarkers of airway inflammation, were not
significantly correlated with ICS treatment response. Explanation for this divergence in
findings is unclear. PRICE results were presented at the May 2005 American Thoracic Society
Annual Meeting
In the Genetics of Asthma in Latino Americans (GALA) study, two ACRN centers compared
asthma-related clinical characteristics of 684 Mexican and Puerto Rican asthmatics recruited
from San Francisco, New York City, Puerto Rico, and Mexico City. Results of the published
study indicate that asthmatic Puerto Ricans had reduced lung function, greater morbidity,
and longer asthma duration than asthmatic Mexicans.
The ACRN was renewed in September 2003 through July 2008. New protocols are under
development and underway.
The Long Acting Beta Agonist Response by GEnotype (LARGE) study is the first protocol of
ACRN II. It is a 60-week randomized, double-blind, cross-over study to compare the effects
of long-acting beta-agonists in patients with asthma who are receiving inhaled
corticosteroids and who express two distinct polymorphisms of the beta2-adrenergic receptor.
The primary hypothesis is that those with the B16 Arg/Arg genotype will have worse asthma
control, as defined by AM PEF rate, than those with the B16 Guj/Guj genotype. Recruitment
started in December 2004 with a target of 80 randomized patients. See NCT00200967 for more
information on this study.
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