A Safety and Efficacy Study of Ciclesonide Nasal Aerosol in Subjects 6-11 Years With Seasonal Allergic Rhinitis (SAR)

Phase 3

Completed

Conditions: Seasonal Allergic Rhinitis

Interventions: Drug: Ciclesonide nasal aerosol 37 mcg
Drug: Placebo
Drug: ciclesonide nasal aerosol 74 mcg

Registration Number: NCT01458275

Lead Sponsor: Sumitomo Pharma America, Inc.

Brief Summary: This is a 2-week, multicenter, randomized, double-blind, placebo-controlled, parallel group, efficacy and safety study of ciclesonide nasal aerosol administered once daily to male and premenarchal female subjects 6 to 11 years-old diagnosed with SAR.

Detailed Description: This is a 2-week, multicenter, randomized, double-blind, placebo-controlled, parallel group, efficacy and safety study of ciclesonide nasal aerosol administered once daily to male and premenarchal female subjects 6 to 11 years-old diagnosed with SAR.

This study will consist of the following:

Screening, Single-blind Placebo Run-in period, Double-blind Treatment period (during this period, subjects will be randomized to double-blind treatment with either ciclesonide nasal aerosol 37 mcg or 74 mcg or placebo for 2 weeks of treatment) and Follow-up. The total duration of subject participation will be approximately 2 months.

Recruitment & Eligibility

Status: COMPLETED

Sex: All

Target Recruitment: 847

Inclusion Criteria

Gives written informed consent (parent/legal guardian) and assent (from the child), including privacy authorization as well as adherence to concomitant medication withholding periods, prior to participation.
Is a male or premenarchal female 6 to 11 years-old at the screening.
Is in general good health (defined as the absence of any clinically relevant abnormalities as determined by the investigator) based on screening physical examination and medical history.
Has a history of SAR to any relevant dominant seasonal allergen for a minimum of one to two years immediately preceding the study Screening Visit. The SAR must have been of sufficient severity to have required treatment (either continuous or intermittent) in the past and is expected to require treatment throughout the entire study period.
Has a demonstrated sensitivity to a relevant dominant seasonal allergen known to induce SAR based on a documented result with a standard skin prick test either within 12 months prior to screening or performed at the screening visit. A positive test is defined as a wheal diameter at least 3 mm larger than the control wheal (normal saline) for the skin prick test. The subject's positive allergen test must be consistent with the medical history of SAR, and the allergen must be present in the subject's environment throughout the study.
Subject or parent/guardian must possess an educational level and degree of understanding of English that enables them to communicate suitably with the Investigator and study coordinator as well as accurately complete both the Allergic Rhinitis diary and Pediatric Rhinoconjunctivitis Quality of Life Questionnaire (PRQLQ).

Exclusion Criteria

Has a history of physical findings of nasal pathology, including nasal polyps or other clinically significant respiratory tract malformations; recent unhealed nasal biopsy; nasal trauma; or nasal ulcers or perforations. Surgery and atrophic rhinitis or rhinitis medicamentosa are not permitted within the 120 days prior to the screening visit.
Has evidence of infection, significant anatomic abnormality, ulceration of the mucosa, blood in the nose, or any other clinically relevant finding on nasal examination at the screening visit.
Has nasal jewelry
Has participated in any investigational drug trial within the 30 days preceding the screening visit or is planning participation in another investigational drug trial at any time during this trial.
Has a known hypersensitivity to any corticosteroid or any of the excipients in the formulation of ciclesonide.
Has a history of a respiratory infection or disorder, including but not limited to bronchitis, pneumonia, influenza, and severe acute respiratory syndrome (SARS), within the 14 days preceding the screening visit.
Has active asthma requiring treatment with inhaled or systemic corticosteroids and/or routine use of beta-agonists and any controller drugs (eg, theophylline, leukotriene antagonists); intermittent use (≤ 3 uses per week) of inhaled short-acting beta-agonists is acceptable. Use of short-acting beta agonists for exercise induced bronchospasm will be allowed.
Plans to travel outside the study area (the known pollen area for the investigative site) for 2 or more consecutive days between Randomization Visit and the final Treatment Visit.
Plans to leave the study area (the known pollen area for the investigative site) for longer than 24 hours during the Single-blind Placebo Run-in period.
Is expecting to use any disallowed concomitant medications during the treatment period.
Is planning initiation of immunotherapy during the study period or dose escalation during the study period. However, initiation of immunotherapy 90 days or more prior to the screening visit and use of a stable (maintenance) dose (30 days or more) may be considered for inclusion.
Has nonvaccinated exposure to or active infection with chickenpox or measles within the 21 days preceding the screening visit.
Initiates pimecrolimus cream 1% or greater or tacrolimus ointment 0.03% or greater during the study period or plans a dose escalation during the study period. However, initiation of these creams/ointments 30 days or more prior to screening and use of a stable (maintenance) dose during the study period may be considered for inclusion.
Is a child or relative of any clinical investigator or site personnel, even those who are not directly involved in this study.
Has any of the following conditions that are judged by the investigator to be clinically significant and/or to affect the subject's ability to participate in the clinical trial: impaired hepatic function; history of ocular disturbances, eg, glaucoma or posterior subcapsular cataracts or herpes simplex; any systemic infection hematological (including anemia), hepatic, renal, endocrine disease; gastrointestinal disease; malignancy (excluding basal cell carcinoma); current neuropsychological condition with or without drug therapy. Any behavioral condition that could affect subject's ability to accurately report symptoms to the caregiver such as developmental delay, attention deficit disorder, and autism.
Has any condition that, in the judgment of the investigator, would preclude the subject from completing the protocol with capture of the assessments as written.
Has received ciclesonide nasal aerosol in a previous clinical trial

Study & Design

Study Type: INTERVENTIONAL

Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
ciclesonide nasal aerosol 37mcg	Ciclesonide nasal aerosol 37 mcg	ciclesonide nasal aerosol 37mcg - the dose is administered as 1 actuation per nostril to give a total dose of 37 mcg
Placebo	Placebo	-
ciclesonide nasal aerosol 74 mcg	ciclesonide nasal aerosol 74 mcg	ciclesonide nasal aerosol 74 mcg - the dose is administered as 1 actuation per nostril to give a total dose of 74 mcg

Primary Outcome Measures

Name	Time	Method
Change From Baseline in Average Daily Subject Reported AM and PM Reflective Total Nasal Symptom Scores (rTNSS) Over the 2-week Double-blind Treatment Period	Weeks 0 - 2	TNSS is the sum of individual symptoms of runny nose, sneezing, itchy nose, and nasal congestions. Subjects assess each individual symptoms on a scale of 0-3 where: 0 = absent 1 = mild 2 = moderate 3 = severe. Therefore, rTNSS values range from 0-12 (with 0 representing an absence of symptoms and higher scores reflecting more severe symptoms). Reflective TNSS measures these symptoms over the previous 12-hour time interval. Difference was calculated as the two week treatment average - baseline. Greater reductions in the change from baseline score indicate greater improvement.

Secondary Outcome Measures

Name	Time	Method
Change From Baseline in Average Daily Subject-reported AM and PM Instantaneous Total Nasal Symptom Scores (iTNSS) Over the 2-week Double-blind Treatment Period	Weeks 0 - 2	TNSS is the sum of individual symptoms of runny nose, sneezing, itchy nose, and nasal congestions. Subjects assess each individual symptoms on a scale of 0-3 where: 0 = absent 1 = mild 2 = moderate 3 = severe Therefore, iTNSS values range from 0-12 (with 0 representing an absence of symptoms and higher scores reflecting more severe symptoms). Instantaneous TNSS measures these symptoms over the previous 10 minute time interval. Difference was calculated as the two week treatment average - baseline. Greater reductions in the change from baseline score indicate greater improvement.
Change From Baseline in Average Daily Subject-reported AM and PM Reflective Total Ocular Symptom Scores (rTOSS) Over the 2-week Double-blind Treatment Period.	Weeks 0 - 2	TOSS is the sum of individual ocular symptoms of itching, tearing, and redness. Subjects assess each individual symptoms on a scale of 0-3 where: 0 = absent 1. = mild 2. = moderate 3. = severe Therefore, TOSS ranges from 0-9 (with 0 representing an absence of symptoms and higher scores reflecting more severe symptoms). Reflective TOSS symptom scores assess symptoms over the previous 12-hour time interval. Difference was calculated as the two week treatment average - baseline. Greater reductions in the change from baseline score indicate greater improvement.
Change From Baseline in the Pediatric Rhinoconjunctivitis Quality of Life Questionnaire (PRQLQ) Overall Score at the End of the Double-blind Treatment Period.	Weeks 0 - 2	PRQLQ was developed to measure the functional problems (physical, emotional, and social) that are most troublesome to children with rhinoconjunctivitis. The PRQLQ has 23 questions in 5 domains (nose symptoms, eye symptoms, practical problems, activity limitation, and other symptoms). Children recalled how they were during the previous week and responded to each question on a 7-point scale (0 = not bothered to 6 = extremely bothered or 0 = none of the time to 6 = all of the time) for a total possible score of 138. The overall PRQLQ score is the mean of all 23 responses and the individual domain scores are the means of the items in those domains.
Change From Baseline in Average Daily Subject Reported AM Instantaneous Total Nasal Symptom Scores (iTNSS) Over the 2-week Double-blind Treatment Period	Weeks 0 - 2	TNSS is the sum of individual symptoms of runny nose, sneezing, itchy nose, and nasal congestions assessed in the AM. Subjects assess each individual symptoms on a scale of 0-3 where: 0 = absent 1 = mild 2 = moderate 3 = severe in the AM. Therefore, iTNSS values range from 0-12 (with 0 representing an absence of symptoms and higher scores reflecting more severe symptoms). Instantaneous TNSS measures these symptoms over the previous 10 minute time interval. Difference was calculated as the two week treatment average - baseline. Greater reductions in the change from baseline score indicate greater improvement.
Change From Baseline in Average Daily Subject-reported AM and PM Instantaneous Total Ocular Symptom Scores (iTOSS) Over the 2-week Double-blind Treatment Period.	Weeks 0 - 2	TOSS is the sum of individual ocular symptoms of itching, tearing, and redness. Subjects assess each individual symptoms on a scale of 0-3 where: 0 = absent 1. = mild 2. = moderate 3. = severe Therefore, TOSS ranges from 0-9 (with 0 representing an absence of symptoms and higher scores reflecting more severe symptoms). Instantaneous TOSS symptom scores assess symptoms over the previous 10 minute time interval. Difference was calculated as the two week treatment average - baseline. Greater reductions in the change from baseline score indicate greater improvement
Time to Maximal Effect in the AM and PM Reflective Total Nasal Symptom Scores (rTNSS) Over the 2-week Double-blind Treatment Period	Weeks 0 - 2	The time to maximal effect, defined as the number of days until the first treatment day on which the estimated difference between ciclesonide nasal aerosol and placebo was at least 90% of the largest estimated difference, was based on the analyses of change from baseline in the average of AM and PM rTNSS scores for each day. The time to achieve at least 90% of these estimated differences is presented.
Number of Subjects Experiencing Treatment-emergent AEs	Weeks 0 - 3	Treatment-Emergent Adverse Events Occurring in ≥ 2% of Subjects in Any Treatment Group (ITT Population)
Percentage of Subjects Experiencing Treatment-emergent AEs	Weeks 0 - 3	Treatment-Emergent Adverse Events Occurring in ≥ 2% of Subjects in Any Treatment Group (ITT Population)
Treatment-emergent AEs Causing Study Medication Discontinuation	Weeks 0 - 3
Number of Subjects Experiencing Treatment-emergent Nasal AEs, Including Epistaxis, Nasal Ulceration, and Nasal Perforation	Weeks 0 - 3
Percentage of Subjects Experiencing Treatment-emergent Nasal AEs, Including Epistaxis, Nasal Ulceration, and Nasal Perforation	Weeks 0 - 3

Trial Locations

Locations (64): Dallas Allergy Immunology Research
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Dallas, Texas, United States
Kerrville Research Associates
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Kerrville, Texas, United States
San Jose Multispecialty Medical Group, Inc
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Baldwin Park, California, United States
Premier Health Research Center
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Downey, California, United States
Center for Clinical Trials, LLC
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Paramount, California, United States
Aeroallergy Research Laboratories of Savannah, Inc
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Savannah, Georgia, United States
Clinical Research Institute of Southern Oregon, PC
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Medford, Oregon, United States
Allergy Associates Research Center
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Portland, Oregon, United States
Storms Clinical Research Institute
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Colorado Springs, Colorado, United States
Pediatric Care Medical Group, Inc.
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Huntington Beach, California, United States
Peninsula Research Associates
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Rolling Hills Estates, California, United States
Northeast Georgia Research Center
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Gainesville, Georgia, United States
Arkansas Pediatric Clinic
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Little Rock, Arkansas, United States
WCCT Global, LLC
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Costa Mesa, California, United States
Catalyst Medical Center
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Fargo, North Dakota, United States
Baker Allergy Asthma and Dermatology Research Center LLC
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Lake Oswego, Oregon, United States
Allergy, Asthma, Brochitis and Immunology Assoc Medical Group
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Fountain Valley, California, United States
Asthma and Allergy Research Associates
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Upland, Pennsylvania, United States
Capital Allergy & Respiratory Disease Center
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Sacramento, California, United States
Isis Clinical Research, LLC
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Austin, Texas, United States
Allergy and Asthma Associates of Southern California
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Mission Viejo, California, United States
Toledo Center for Clinical Research
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Sylvania, Ohio, United States
Allergy Associates Medical Group
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San Diego, California, United States
Atlanta Allergy & Astma Clinic
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Marietta, Georgia, United States
Asthma & Allergy Associates, PC
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Colorado Springs, Colorado, United States
DCT - Barlite Dba Discovery Clinical Trials
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San Antonio, Texas, United States
San Antonio Ear, Nose & Throat Research
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San Antonio, Texas, United States
Research Across America
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Carroliton, Texas, United States
Sylvana Research Associates
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San Antonio, Texas, United States
Live Oak Allergy and Asthma Clinic
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Live Oak, Texas, United States
Sun Research Institute
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San Antonio, Texas, United States
North Texas Family Medicine
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Plano, Texas, United States
Allergy & Asthma Care of Waco
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Waco, Texas, United States
Spartanburg Medical Research
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Spartanburg, South Carolina, United States
Sirius Clinical Research LLC
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Austin, Texas, United States
Central Texas Health Research
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New Braunfels, Texas, United States
Allergy Asthma Research Institute
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Waco, Texas, United States
Pediatric Care Medical Group
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Huntington Beach, California, United States
CHOC, PSF, AMC, Division of Allergy, Asthma, and Immunology
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Orange, California, United States
Allergy & Asthma Medical Group and Research Center, APC
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San Diego, California, United States
Bensch Research Associates
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Stockton, California, United States
Colorado Allergy and Asthma Centers, PC
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Denver, Colorado, United States
DataQuest Medical Research, LLC
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Lawerenceville, Georgia, United States
Sneeze, Weeze, & Itch Associates
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Normal, Illinois, United States
Alzein Pediatrics
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Evergreen Park, Illinois, United States
Gordon D. Raphael, MD
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Berthesda, Maryland, United States
Creighton University Medical Center
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Omaha, Nebraska, United States
Clinical Research Institute
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Plymouth, Minnesota, United States
North Carolina Clinical Research
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Raleigh, North Carolina, United States
Atlantic Research Center, LLC
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Ocean, New Jersey, United States
Discovery Clinical Trials
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Arlington, Texas, United States
Asthma, Nasal Disease & Allergy Research Center of New England
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Providence, Rhode Island, United States
National Allergy, Asthma, and Uticaria Centers of Charleston, PA
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Charleston, South Carolina, United States
Benchmark Research
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San Angelo, Texas, United States
TTS Research Center
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Boeme, Texas, United States
Western Sky Medical Research
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El Paso, Texas, United States
DCT - Anchor, LLC dba Discovery Clinical Trials
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Arlington, Texas, United States
Pharmaceutical Research and Consulting
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Dallas, Texas, United States
ACRC Trials
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Plano, Texas, United States
Allergy and Asthma Research Center, PA
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San Antonio, Texas, United States
DCT-Westover Hills, Dba Discovery Clinical Trials
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San Antonio, Texas, United States
Pediatric Healthcare of Northwest Houston
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Tomball, Texas, United States
Ericksen Research and Development
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Clinton, Utah, United States
Clinical Research Atlanta
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Stockbridge, Georgia, United States