Role of Immunoglobulin E (IgE) Bearing Cells in Chronic Idiopathic Urticaria (CIU)



Status:Recruiting
Conditions:Dermatology
Therapuetic Areas:Dermatology / Plastic Surgery
Healthy:No
Age Range:18 - 65
Updated:10/11/2018
Start Date:October 6, 2017
End Date:May 31, 2019
Contact:Kelly Devine, RN
Email:ssaini@jhmi.edu
Phone:410-550-2129

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Role of Immunoglobulin E (IgE) Bearing Cells in Chronic Idiopathic Urticaria

This is a Phase IV, single-site study that will examine blood cells or tissue obtained from
CIU patients receiving open-label treatment with omalizumab at the current FDA-approved dose
of 300 mg/month for 12 weeks in addition to standard therapy with anti-histamines. Results
from the 3 Phase III studies in CIU patients provide evidence that a meaningful change in
symptoms is apparent at 1-2 wks. The Minimal Important Difference (MID) is achieved by 70% of
patients by 2 wks on multiple background drugs for hives. The goal is to identity the IgE
bearing cell type associated with clinical symptom change.

Primary Objective

This will be a study of the kinetics of clinical symptom relief during treatment of patients
with CIU. The purpose is to determine if the rate of clinical remission is concordant with
the rate that IgE-dependent functions of basophil change or mast cell changes during
treatment.

Secondary Objectives

1. Basophil surface IgE, Fc epsilon Receptor I alpha (FcεRI) and Syk by flow cytometry

2. Dendritic cell surface IgE, FcεRI, functions

3. Basophil anti-IgE, anti FcεRI, C5a, N-Formylmethionyl-leucyl-phenylalanine (FMLP)
mediated histamine along with sensitivity measures

4. Serum free IgE measures

5. Characterization of presence of serum autoantibody presence ± Syk inhibitors

6. Basophil enumeration

7. Basophil Messenger RNA (mRNA) profiling baseline at 3 timepoints (baseline, meaningful
clinical changes, and 30 days)

8. To assess the rate of IgE and FcεRI change in skin mast cells at day 0, 6, 90, via a
small punch biopsy as well as the Mas-Related gpr Family Member X2 (MrgX2) receptor
expression

Study Design

This is a Phase IV, single-site study that will examine blood cells or tissue obtained from
CIU patients receiving open-label treatment with omalizumab at the current FDA-approved dose
of 300 mg/month for 12 weeks in addition to standard therapy with anti-histamines. Results
from the 3 Phase III studies in CIU patients provide evidence that a meaningful change in
symptoms is apparent at 1-2 wks. The MID (Minimal Important Difference) is achieved by 70% of
patients by 2 wks on multiple background drugs for hives. The goal is to identity the IgE
bearing cell type associated with clinical symptom change.

The study will enroll 30 patients and will consist of three phases.

Screening Visit (Week -3 to Week-2)-establish compliance with diary and review safety labs.

Standard therapy Run-in (Week -2 to Day 0)

Open-label Treatment Period (Day 0 to Week 12)

To be eligible at the screening visit (Week -1), subjects must:

1. Be 18−65 years old

2. Have a diagnosis of moderate to severe CIU, as defined by pruritus and hives for > 3
days in a 7-day period for > 6 consecutive weeks despite treatment with H1
antihistamine:

Must have a non-diary based daily urticaria activity score (UAS) score ≥ 2 established in the
outpatient setting based on the patient's condition over 12 hours prior to the visit; the UAS
is a composite score of pruritus (0-3) and number of hives (0-3) with a maximum value of 6.

This requirement may be met either at screening visit, run-in visit (Week -2), or beginning
of treatment (Day 0).

Must have been on an approved dose of an H1 antihistamine for CIU such as loratadine 10 mg
once a day or equivalent, for at least 7 days prior to the screening visit. Approved agents
include loratadine 10 qd, desloratadine 5 mg qd, fexofenadine 180 mg qd, cetirizine 10 mg qd
or levocetirizine 5 mg qd as once daily medications at the current FDA-approved dose.

Must be willing to fill out a twice-daily patient-diary to establish the patient's Urticaria
Activity Score 7 (UAS7) score. The UAS is a composite diary- recorded score with numeric
severity intensity ratings (0 = none to 3 = intense) for 1) the number of wheals (hives); and
2) the intensity of the pruritus (itch). The UAS7 is the sum of the daily average UAS scores
(average of a.m. and p.m.) for 7 days. The maximum UAS7 value is 42.

To be eligible to begin the run-in period (Week -2 to Day 0), the patients:

Must remain on stable dose of a single H1 antihistamine at approved dose (not including
antihistamine rescue medication) as established at the screening visit.

At the end of the 12-week treatment period , subjects will have last visit a final visit to
collect diary, blood work, non-lesional skin biopsy and safety data.

All patients will be provided diphenhydramine (25 mg po TID) as rescue medication for
pruritus relief on an as-needed basis (to a maximum of three doses in 24 hours). Patients who
require treatments other than diphenhydramine (e.g., prednisone) to treat
persistent/worsening disease will be discontinued from the study. Patients will also be
provided an epipen and trained in its use as per American Academy of Allergy, Asthma &
Immunology (AAAAI) guidelines for omalizumab.

Primary Endpoint The time to meaningful change in diary-based clinical symptoms as measured
by the Urticaria Activity Score from baseline (Wk -7 to Day -1) to the date at which an MID
(5 point change in weekly UAS 7) or achievement of > 50% reduction in daily symptom score for
3 days if in the first week. The UAS score, which is the sum of pruritus and hives, will be
used to calculate the UAS7. The UAS7 score obtained 1 week prior to randomization will be
used as the baseline.

Secondary Endpoints

Change in the weekly pruritus score from baseline to the 12th week in the treatment period.
The pruritus score will be measured twice daily (a.m. and p.m.), on a scale of 0 (none) to 3
(intense). The weekly pruritus score is the sum of average daily pruritus scores over the
previous 7 days.

Change in the weekly score for number of hives from baseline to the 12th week in the
treatment period. The number of hives is measured twice daily (a.m. and p.m.), on a scale of
0 (none) to 3 (> 12 hives, see below). The weekly score of number of hives is the sum of the
average daily scores over the previous 7 days.

Change in the amount of rescue medication (diphenhydramine 25 mg) from baseline to the 12th
week in the treatment period using the question on the rescue medication use in the patient
diary.

Change in SKINDEX29 quality of life survey instrument with 29 questions on a 5-point Likert
scale. It will be given at baseline and again at 90 days.

Exploratory Endpoints

1. Basophil surface IgE, FcεRI and Syk by flow cytometry- Day 0, 1, 3, 6, 10, 20, 30 and 90
days

2. Dendritic cell surface IgE, FcεRI -Day 0, 1, 3, 6, 10, 20, 30 and 90 days

3. Basophil anti-IgE, anti FcεRI, C5a, FMLP mediated histamine release along with
sensitivity measures- Day 0, 1, 3, 6, 10, 20, 30 and 90 days

4. Serum free IgE measures (stored serum) Day 0, 1, 3, 6, 10, 20, 30 and 90 days

5. Characterization of presence of serum autoantibody presence ± Syk inhibitors -Day 0, 1,
3, 6, 10, 20, 30 and 90 days

6. Basophil enumeration by manual counting and blood histamine content - Day 0, 1, 3, 6,
10, 20, 30 and 90 days. This will determine the presence or absence of basopenia and
identify subjects for mRNA profiling studies.

7. Basophil mRNA profiling baseline at 3 timepoints (baseline, meaningful clinical changes,
and 30 days) in select subjects with sufficient basophil numbers ( >1.5x 106/100 cc
blood)

8. Numbers of IgE +, FcεRI + cells in non-lesional skin biopsies at day 0, 6, 90 to monitor
skin mast cells well as the MrgX2 receptor expression

9. Change in circulating leukocyte population numbers that are targeted by omalizumab such
as blood basophils, eosinophil and lymphocyte counts by automated analysis (week -3 to
week 12).

Inclusion Criteria:

- Male or female, ages 18-65

- Females must be surgically sterile or postmenopausal or using a highly effective form
of birth control throughout the duration of the study.

- Females must have a negative urine pregnancy test at screening and other visits
specified in this protocol unless documented to have a hysterectomy or be
postmenopausal.

- Clinical history of CIU at the time of screening, as defined by pruritus and hives for
> 3 days in a 7-day period for > 6 consecutive weeks despite treatment with H1
antihistamine.

- CIU diagnosis > 3 months (by history)

- No underlying etiology clearly defined for urticaria (main manifestation cannot be
physical urticaria).

- Non-diary based UAS scores ≥ 2 at either the screening visit (Week -3), at the run-in
visit (Week -2), or on Day 1.

- Compliance with study procedures during run-in period (e.g., completion of the study
diary).

Exclusion Criteria:

- Pregnant females, Recent history of drug or alcohol abuse (within 3 years prior to
screening visit).Inability or unwillingness of a participant to give written informed
consent or comply with study protocol.

- Use of any investigational drugs within 30 days of screening.

- Active atopic dermatitis or other skin disease associated with pruritus during the
time of the study, which require treatment with topical corticosteroids.

- Clinically relevant major systemic disease (making interpretation of the study results
difficult) including a history of anaphylaxis.

- Inability to comply with study and follow-up procedures

- Patients may not use oral or systemic steroids during the study or within 4 weeks
prior to enrollment.

- Patients may not take H2 antihistamines and leukotriene receptor antagonists within 7
days before screening, during the screening, run-in, or treatment phases. The
exception will be if they are already on these medications for the treatment of
Gastro-Esophageal Reflux Disease (GERD), asthma or allergic rhinitis.

- Any clinically relevant abnormal findings in clinical chemistry, hematology,
urinalysis, physical examination, pulse, blood pressure at baseline, which, in the
opinion of the investigator, could put the patient at risk because of his/her
participation in the study.

- Past or current medical problems or findings from physical examination or laboratory
testing that are not listed above, which, in the opinion of the investigator, may pose
additional risks from participation in the study, may interfere with the participant's
ability to comply with study requirements or may compromise the quality of the data
obtained from the study.
We found this trial at
1
site
Baltimore, Maryland 21224
Principal Investigator: Sarbjit S Saini, M.D.
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mi
from
Baltimore, MD
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