Chronic Spontaneous Urticaria Clinical Trial
Official title:
Prospective Double-blind Placebo-controlled Study of the Effect of Xolair (Omalizumab) in Chronic Urticaria Patients
The aim of this study is to investigate the pathophysiological mechanism of omalizumab in patients with documented chronic urticaria who have complaints under standard antihistamine treatment. With this study the investigators will assess the correlation between Fc-IgE receptor downregulation as well as functionality and clinical response to omalizumab treatment in patients with chronic urticaria. This may be an approach for other diseases as well, where Fc-IgE receptor crosslinking are essential. The treatment time is set for a total of 4 monthly applications of omalizumab. According to the dosage recommendations of recent studies, fixed doses of 300 mg omalizumab are administered subcutaneously.
Background
Chronic urticaria (CU) is a frequent disease with a lifetime incidence of up to 25-30% of
the population. Currently, CU treatment relies mainly on second generation antihistamines
and is purely symptomatic. The disease tends to have a cyclical nature with spontaneous
disappearance and frequent relapses. Some patients show a sufficient response to standard
second generation antihistamines like (levo)cetirizine 10mg, (des)loratadine 5mg or
terfenadine 120-180mg. Others need higher doses (up to 4-fold usual daily dose), often
accompanied by sedation. Treatment may last for months, even years. If this first-line
therapy is insufficient, the next step (sometimes even before use of excessively high doses
of antihistamines) is to add first generation, even more sedating antihistamines, some of
which have additional modes of action (e.g. anticholinergic effects in doxepin treatment). A
considerable number of patients with CU need treatment escalations with leukotriene receptor
blocking agents (e.g. montelukast), systemic corticosteroids (5-20mg prednisolon/d) or even
cyclosporine (daily dose 3-5 mg/kg) or other immunosuppressive drugs used off-label. Such
patients are often investigated more in detail to find an infection or autoimmune disease -
often still without clear results.
Different clinical findings suggest that the mast cell system in many patients with CU is
"overactive" with increased releasability. Minor stress like scratching can already induce
degranulation resulting in wheal-and-flare skin reactions. Therefore, a therapy directly
aiming at a decrease in this mast cell "hyperreleasability" would be optimal. Omalizumab
binds selectively to free IgE in plasma, inhibits its binding to Fc-IgE receptor on the
surface of mast cells and basophils and reduces the number of Fc-IgE receptors on basophils
in atopic patients. Significant reduction of Fc-IgE receptor density on the surface of
circulating basophils has been found as early as 1 week after administration of omalizumab.
In contrast to this, the onset of clinical efficacy of omalizumab in asthma is considered to
take place relatively late, namely about 4 months after start of treatment. The
pathophysiologic concepts of omalizumab treatment in allergic asthma are focused on the
neutralisation of IgE, and less on the Fc-IgE receptor density. In allergology, free IgE in
plasma is only relevant regarding Fc-IgE receptor density on effector cells. Therefore,
Fc-IgE receptor density measurement might be an important parameter for mast cell and
basophil "releasability" and therefore a good in vitro surrogate marker for their
reactivity. E.g. it is well known that only about 50% of IgE-sensitized individuals show
clinically relevant allergic symptoms. This difference between sensitization and allergy may
also be due to Fc-IgE receptor density on mast cells and basophils. Flowcytometric
determination of Fc-IgE receptor density on the surface of basophils and additional testing
for the functional consequences of a change in this density (ability to crosslink Fc-IgE
receptors by autoantibodies and allergens) raise the possibility to evaluate this hypothesis
- using omalizumab as a drug being able to decrease Fc-IgE receptor density:
1. Study data show that a fixed dose of 300 mg omalizumab is useful for the treatment of
CU. The investigators assume that this effect is due to the decrease of Fc-IgE receptor
density. Thus, the basophil Fc-IgE receptor density should be monitored quantitatively
and functionally (see below) and correlated to clinical response.
2. 30-40% of patients with CU have autoantibodies against Fc-IgE receptor or IgE itself,
which can be measured in vitro (already via ELISA, flowcytometric via CD63 and CD203c
upregulation on basophils). Decrease of Fc-IgE receptor density may decrease basophil
reactivity and explain or be correlated to the clinical response in CU patients. At
least three patients will be followed for reactivity to autoantibodies over the study
period.
3. Some patients with CU may also have an accompanying IgE-mediated allergy, which is most
probably irrelevant for the CU, but offers the possibility of a functional test of
basophil responsiveness to low concentrations of allergens - before (with presumably
high Fc-IgE receptor density) and after omalizumab treatment (low Fc-IgE rec. density).
At least three patients will be followed for allergen reactivity of basophils.
Objective
Primary objectives
− Measurement of the kinetic of Fc-IgE receptor density change on basophils from patients
with chronic urticaria with omalizumab compared to placebo
Secondary objectives
- Change of responsiveness to Fc-IgE cross-linking dependent stimuli:
- incubation of patient's basophils with anti-IgE
- allergen induced cross-linking (only grass pollen and birch pollen allergic
patients)
- comparison of serum on third party basophils
- Measurement of IL-3 hyperresponsiveness of basophils after Stimulation with anti-IgE
and allergen
- Daily urticaria activity score
- Medication and rescue medication use
- German version of the Chronic Urticaria Quality of Life Questionnaire (CU-Q2oL)
Methods
This is a monocentric, double-blind, randomized placebo-controlled trial, which aims to
investigate the pathophysiological mechanism of omalizumab in patients with documented
chronic urticaria who have complaints under standard antihistamine treatment.
According to the inclusion criteria, 30 patients with diagnosed chronic urticaria will be
recruited in our outpatient clinic. Omalizumab (Xolair®) is administered in fixed dose of
300 mg in a total of 4 monthly doses according to the reference. A follow-up visit is
planned 2 months after the last injection.
;
Allocation: Randomized, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Basic Science
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