Asthma Clinical Trial
Official title:
A Multi-Center, Randomized, Double-Blind, Active-Controlled, Parallel Group, 4-Week Study to Evaluate the Efficacy, Safety and PK of Albuterol-HFA Versus Proventil-HFA in Pediatric Patients With Asthma in Pediatric Patients With Asthma
This 4-week clinical study evaluates the efficacy and safety of Albuterol Sulfate HFA Inhalation Aerosol in comparison with the Active Control, Proventil-HFA (3M Pharmaceuticals, Inc) in pediatric patients (4-11 years old) with mild-to-moderate asthma. In addition, pharmacokinetic profile in this population will be evaluated using a population PK approach with sparse blood samples.
This study consists of two periods:
1. Run-in Period (7-14 days): During the Run-in Period, subjects will maintain their
current inhaled short-acting B2-agonist and inhaled corticosteroid therapies. All
long-acting b-agonists (LABA) will be prohibited and replaced with a short-acting
B2-agonist (Ventolin-HFA) and an inhaled corticosteroid, for a minimum of 7 days. Such
LABA replacement therapy is not considered as violation of the asthma stability. The
current orally inhaled corticosteroids may be maintained at the prescribed dosing
regimen. All concomitant medications must be compliant or adjusted to the restrictions
and washout time limits per Appendix II. Subjects will document their daily asthma
symptom scores, treatment regimens, concomitant medications, PEF records, and adverse
events if any.
2. Study Period (4 wk): During the 4-week Study Period, subjects will be randomized into
one of the following 2 double-blinded treatment groups:
- Treatment T (Albuterol-HFA, N=24): 216 mcg albuterol sulfate (equivalent to 180
mcg albuterol base), oral inhalation, QID;
- Treatment R (Proventil-HFA, N=24): 216 mcg albuterol sulfate (equivalent to 180
mcg albuterol base), oral inhalation, QID.
During the Study Period, subjects will document their daily asthma symptom scores, treatment
regimens, concomitant medications, PEF records, and adverse events if any. Three Clinical
Visits are to be conducted, for measurement of treatment efficacy with serial spirometry (at
Clinical Visit 1 and 3); for monitoring safety and compliance (at Clinical Visit 1, 2 and
3); and for evaluating pharmacokinetic profiles in part of the study population (greater
than or equal to 6 subjects per Arm) using a population PK approach (PPK) with a sparse
blood sampling regimen (at Clinical Visit 3).
STUDY POPULATION
Sufficient enrollment will be planned to obtain 48 subjects as "Per protocol population",
with 24 in Albuterol-HFA (Arm T) and 24 in the Proventil-HFA (Arm R). Qualified subjects
should be:
1. Male and female patients aged 4 - 11 years (upon screening), and female patients being
premenarchal upon Visit-1.
2. With documented mild-to-moderate asthma for at least 6 months prior to screening;
3. Being able to reliably perform spirometric FEV1 test;
4. Consent, under supervision of a parent or a legal guardian, to participate in the
study;
5. Having a baseline forced expiratory volume in 1 second (FEV1) that is 50.0%-100.0% of
predicted values at screening (Screening Baseline FEV1);
6. Demonstrating a greater than or equal to 12.0% FEV1 reversibility in the Reversibility
Test, at 30 min after inhaling 180 mcg of Ventolin-HFA;
7. Satisfying the criterion of asthma stability, defined as no significant changes in
asthma therapy and no asthma-related hospitalization or emergency visits, over 4 weeks
prior to the screening;
8. Satisfying the Run-in Period requirements;
9. Satisfying all other inclusion/exclusion criteria, as specified in Section 4.2.
TREATMENT REGIMENS
Enrolled subjects will be randomized to receive one of the 2 double-blinded treatments:
Albuterol-HFA (Treatment T) or Proventil-HFA (Treatment R).
CLINICAL VISITS:
The entire study consists of a Screening Period, a Run-in Period, and a Study Period which
consists of three (3) Clinical Visits. The three (3) Clinical Visits are scheduled with 14±3
days intervals, as Visit 1 (Day 0 of treatment), Visit 2 (Day 14), and Visit 3 (Day 28). The
Clinical Visit 1 will be held within 7-14 days after Screening Visit. Serial FEV1 are
performed at Visit 1 and 3. Safety and compliance are evaluated at all 3 Visits. Population
PK (PPK) blood sampling is conducted at Visit 3.
METHODOLOGIES AND SPECIFIC MEASUREMENTS
1. Forced Expiratory Volume at 1st Second (FEV1)
Spirometry is to be used to determine Forced Expiratory Volume in the 1st second
(FEV1). Patient may choose either a standing or a sitting position for FEV1. The
position, once chosen, should be kept consistent for the entire study. Nose clips will
be worn for the FEV1 measurements.
Each FEV1 is measured in triplicate at a given test or a given time point. The highest
FEV1 volume, from the triplicate attempts, is used as the representative value. The
highest and second highest FEV1 attempts should not differ by greater than 0.2 L. Up to
2 additional attempts may be measured if necessary, with a total of 3-5 attempts
allowed for a given test. The accepted attempts have to be technically conforming to
the current spirometry standards from the American Thoracic Society (ATS). The current
clinical normative lung volumes in conformity with the ATS guidelines will be used for
calculating the predicted percentage.
2. Peak Expiratory Flow (PEF) Rate
PEF will be measured as a means of monitoring safety and asthma control. PEF will be
measured in triplicate, with additional attempts if necessary. The highest PEF volume is
used as the representative value. Two measurements of PEF are made daily, once prior to the
first AM dose and once prior to the last PM dose of the study drug. Subject will be standing
for PEF measurements. No nose-clips will be needed for PEF.
2) Screening Baseline FEV1
Passing the Screening Baseline FEV1 test is one of the prerequisites for enrollment, and is
to be conducted at the Screening Visit by all subjects. The Screening Baseline FEV1 should
fall within 50.0%-100.0% of the predicted value to qualify the subject.
3) Reversibility FEV1 Test
Reversibility FEV1 Test will be performed at the Screening Visit. Within 30 min after the
Screening Baseline FEV1 is obtained, the subject will self-administer 180 to 360 mcg
Ventolin-HFA (2-4 inhalations). To qualify for the study, the subject needs to demonstrate
an FEV1 reversibility of greater than or equal to 12.0%, from the (same-day) Screening
Baseline FEV1, with 3 to 8 attempts, at 30 min after inhaling Ventolin-HFA. Reversibility is
defined as:
% Reversibility = [(FEV1 postdose ~ FEV1 predose)/FEV1 predose] x 100%
Up to two-time re-tests of the Reversibility FEV1 Test will be allowed if the highest
attempted reversibility value is less than 12.0% but greater than or equal to 6.0, if deemed
necessary by the investigator, with screening period extendable to a total of 21 days.
4) Serial FEV1 measurements of study drug efficacy
Response to the study drugs (T and R) is examined by serial spirometric measurements of FEV1
post-dose. Serial FEV1 will be conducted at each of the following time points during Study
Visits 1 and 3:
1. at baseline (within 30 minutes prior to study drug dosing).
2. at 10, 30, 45, 60, 120, 180, 240, 300, and 360 minutes after dosing.
POPULATION PHARMACOKINETIC (PPK) EVALUATION
At clinical Visit 3, a sufficient number of patients will be subject to a population
pharmacokinetic (PPK) study to obtain a minimum of 6 subjects per arm with complete and
correct 4 PK samples. An indwelling IV catheter may be used, as an alternative to repeated
venipunctures, for PPK samples. An appropriate anticoagulant may be used to maintain the
catheter patency. Four blood samples (~5.0 mL each) will be taken from a hand or forearm
vein of the subject, at pre-scheduled 4 time points: 2, 4, 6 and 8 hr post-dose (each with a
±15 min window). No inhalation of the study drug or rescue medication should take place
until completion of the 8-hr PK sampling, unless needed for rescue, at which point the
subject will not be considered evaluable for the PK endpoint.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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