Effect of Anti-IgE in Non-Allergic Asthma
| Status: | Recruiting |
|---|---|
| Conditions: | Asthma |
| Therapuetic Areas: | Pulmonary / Respiratory Diseases |
| Healthy: | No |
| Age Range: | 18 - 80 |
| Updated: | 4/2/2016 |
| Start Date: | April 2005 |
| Contact: | Susan L Whaley, MPH |
| Email: | swhaley1@jhmi.edu |
| Phone: | 410-550-2122 |
The purpose of this study is to find out if omalizumab is effective in treating non-allergic
asthma. The US Food and Drug Administration has approved the use of omalizumab to treat
moderate to severe allergic asthma.
asthma. The US Food and Drug Administration has approved the use of omalizumab to treat
moderate to severe allergic asthma.
Asthma is a chronic inflammatory disease of the lower airways. The inflammatory process is
associated with changes in airway hyperresponsiveness (irritability), and airflow
limitations caused by bronchoconstriction, edema, and mucous plugging. Mast cells,
basophils, eosinophils, activated T-lymphocytes, macrophages, neutrophils, and airway
epithelial cells all play a role in this inflammatory process by releasing mediators
directly responsible for local inflammation and by releasing mediators that encourage a
further influx of inflammatory cells (Expert Panel Report 2, 1997). These cells and their
products eventually produce a state of chronic allergic inflammation leading to increased
vascular leakage, mucous secretion, smooth muscle hyperresponsiveness, and nerve activation.
Clinically, this process is characterized by intermittent shortness of breath, wheezing,
coughing, and chest tightness.
Although most asthmatics are atopic (allergic), non-atopic asthmatics exist and can develop
equally severe disease. Non-allergic asthmatics have a trend towards higher than normal
levels of the allergic antibody (IgE) though obviously they lack skin test specificity. When
examining skin test reactivity and serum IgE as independent variables for asthma risk, there
was a stronger association with serum IgE elevation than skin test reactivity. In fact,
serum IgE tended to be high in asthmatics regardless of skin test reactivity.
Omalizumab (Xolair®) is a recombinant humanized monoclonal antibody that binds specifically
to the (FceRI) binding site on human IgE. The binding of omalizumab inhibits the ability of
IgE to bind to basophils or mast cells.
Omalizumab recently received FDA approval for the treatment of moderate to severe persistent
allergic asthma in pediatric (12 years of age and above) and adult patients. The addition of
omalizumab to standard asthma therapies has been found to reduce asthma exacerbations and
decrease both inhaled corticosteroid dose and rescue medication use. (Busse, 2001). In a
phase III double blinded placebo controlled trial involving 525 severe allergic asthmatics,
omalizumab treated patients had fewer exacerbations during both a steroid stable phase and
steroid reduction phase than did placebo controls (Busse, 2001). The median reduction in
steroid dose during reduction phase was 75% and 50% in the omalizumab and placebo groups
respectively. In a similarly designed steroid reduction study involving 6 to 12 year-old
moderate to severe allergic asthmatics, steroid reduction was possible in 100% of treated
patient verses 66.7% of placebo treated patients (Milgrom, 2001). Other steroid reduction
studies have had similar results (Buhl 2002, Soler 2001). Omalizumab has also been shown to
improve quality of life in allergic asthmatics as measured by the Asthma Quality of Life
Questionnaire (AQLQ). In adults, AQLQ demonstrated greater improvement at 16, 28 and 52
weeks in omalizumab treated patients than in placebo treated (Finn 2003). Similarly in
pediatric populations, AQLQ improvement reached statistical significance in omalizumab
treated patients (Lemanske 2002).
Omalizumab has shown itself to be a promising new therapy for the treatment of moderate to
severe allergic asthma. It is currently not indicated for patients with non-allergic asthma.
The objective of this study will be to define the effects of omalizumab on cell surface
FceRI expression and serum IgE of non-allergic asthmatics.
associated with changes in airway hyperresponsiveness (irritability), and airflow
limitations caused by bronchoconstriction, edema, and mucous plugging. Mast cells,
basophils, eosinophils, activated T-lymphocytes, macrophages, neutrophils, and airway
epithelial cells all play a role in this inflammatory process by releasing mediators
directly responsible for local inflammation and by releasing mediators that encourage a
further influx of inflammatory cells (Expert Panel Report 2, 1997). These cells and their
products eventually produce a state of chronic allergic inflammation leading to increased
vascular leakage, mucous secretion, smooth muscle hyperresponsiveness, and nerve activation.
Clinically, this process is characterized by intermittent shortness of breath, wheezing,
coughing, and chest tightness.
Although most asthmatics are atopic (allergic), non-atopic asthmatics exist and can develop
equally severe disease. Non-allergic asthmatics have a trend towards higher than normal
levels of the allergic antibody (IgE) though obviously they lack skin test specificity. When
examining skin test reactivity and serum IgE as independent variables for asthma risk, there
was a stronger association with serum IgE elevation than skin test reactivity. In fact,
serum IgE tended to be high in asthmatics regardless of skin test reactivity.
Omalizumab (Xolair®) is a recombinant humanized monoclonal antibody that binds specifically
to the (FceRI) binding site on human IgE. The binding of omalizumab inhibits the ability of
IgE to bind to basophils or mast cells.
Omalizumab recently received FDA approval for the treatment of moderate to severe persistent
allergic asthma in pediatric (12 years of age and above) and adult patients. The addition of
omalizumab to standard asthma therapies has been found to reduce asthma exacerbations and
decrease both inhaled corticosteroid dose and rescue medication use. (Busse, 2001). In a
phase III double blinded placebo controlled trial involving 525 severe allergic asthmatics,
omalizumab treated patients had fewer exacerbations during both a steroid stable phase and
steroid reduction phase than did placebo controls (Busse, 2001). The median reduction in
steroid dose during reduction phase was 75% and 50% in the omalizumab and placebo groups
respectively. In a similarly designed steroid reduction study involving 6 to 12 year-old
moderate to severe allergic asthmatics, steroid reduction was possible in 100% of treated
patient verses 66.7% of placebo treated patients (Milgrom, 2001). Other steroid reduction
studies have had similar results (Buhl 2002, Soler 2001). Omalizumab has also been shown to
improve quality of life in allergic asthmatics as measured by the Asthma Quality of Life
Questionnaire (AQLQ). In adults, AQLQ demonstrated greater improvement at 16, 28 and 52
weeks in omalizumab treated patients than in placebo treated (Finn 2003). Similarly in
pediatric populations, AQLQ improvement reached statistical significance in omalizumab
treated patients (Lemanske 2002).
Omalizumab has shown itself to be a promising new therapy for the treatment of moderate to
severe allergic asthma. It is currently not indicated for patients with non-allergic asthma.
The objective of this study will be to define the effects of omalizumab on cell surface
FceRI expression and serum IgE of non-allergic asthmatics.
Inclusion Criteria:
- Males and non-pregnant, non-breastfeeding females 18 through 80 years of age
- Clinically acceptable ECG
- Diagnosis of moderate to severe persistent asthma
- History or presence of episodic symptoms of airflow obstruction (wheeze, chest
tightness, cough, shortness of breath)
- Airflow obstruction is at least partially reversible
- FEV1 in the context of this study is <80%of predicted values at visit 1 with no
short-acting ß agonist use within 6 hours of spirometry
- Improvement of at least 12% of predicted FEV1 value and at least 200 ml within 15 to
30 minutes of inhaling nebulized albuterol (up to 5mg) or 2-4 puffs of albuterol (90
mcg/actuation) demonstrated at study entry or documented in the last year.
- Subjects must be able to demonstrate proper technique for use of the MiniWright peak
flow meter
- Subjects must have a negative skin test to the 5 common perennial aeroallergens (D.
farinae, D. pteronyssinus, cat, dog, and cockroach) at prick puncture with an
adequate histamine control.
- Subjects must have negative RAST to the same 5 common perennial aeroallergens .
- Serum total IgE must be 30-700 IU/ml.
- Normal EKG at baseline
- Females must be: Surgically sterile (hysterectomy, bilateral oophorectomy, bilateral
tubal ligation), OR postmenopausal (at least 1 year since last menses), OR using one
of the following medically acceptable forms of birth control throughout the duration
of the study:
- Systemic contraceptives
- Diaphragm with intravaginal spermicide
- Cervical cap
- Intrauterine device
- Condom with intravaginal spermicide
- Females in certain categories (not sexually active, vasectomized partner) will be
admitted at the discretion of the investigator on a case-by-case basis. Accepted
cases will be documented on the Female Enrollment Form and kept with the informed
consent document.
- Females, excluding those more than 1 year postmenopausal or who are surgically
sterile, must have a negative urine pregnancy test at Visit 1 and other visits
specified in this protocol. If a subject becomes pregnant during the study
participation, they will be discharged from the study and followed until termination
of the pregnancy or delivery is complete.
Exclusion Criteria:
- Respiratory tract infection within 14 days prior to Visit 1
- Chronic bronchitis, COPD, emphysema and other chronic lung diseases
- Receiving immunotherapy other than maintenance therapy
- Current smokers
- Current use of Xolair®
- Recent history of drug or alcohol abuse (within 3 years prior to Visit 1)
- Pregnant or likely to become pregnant during the study
- Breast-feeding
- History of hypersensitivity to albuterol, or Xolair, or to drugs with similar
chemical structures
- Treatment with any investigational drug in the last 30 days before enrollment into
the study (Visit 1)
- Clinically relevant cardiovascular, hepatic, neurologic, psychiatric, endocrine, or
other major systemic disease making the protocol or interpretation of the study
results difficult
- Site staff members or their immediate families are not eligible to enroll
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