Dose Finding Study Depigoid Phleum: 4 Doses in Patients With Allergic Rhinitis/Rhinoconjunctivitis +-Asthma

Leti Pharma

Status and phase

Completed

Phase 2

Conditions

Sensitization Against Phleum Pratense Pollen

Allergic Rhinitis/Rhinoconjunctivitis +- Intermittent Asthma

Dose-Finding Study

Treatments

Biological: Depigoid Phleum

Study type

Interventional

Funder types

Industry

Identifiers

NCT01634958

6043-PG-PSC-192

2012-000416-28 (EudraCT Number)

Details and patient eligibility

About

Specific immunotherapy for IgE mediated sensitization to grass pollen

4 concentrations of a modified pollen extract of Phleum pratense are applied to find out the optimum dose.

Full description

This is a dose finding study and no therapeutic study. Patients will receive in 4-weekly intervals 6x 0,5mL of one of 4 different concentrations of Depigoid Phleum. The study is performed outside the pollen season. Thus the aim of the study is not the therapeutic effect of the specific immunotherapy (effect on allergy specific symptoms during the pollen season) but the effect on the Conjunctival provocation test (CPT). According to the EMA "Guideline on clinical development of products for specific immunotherapy for the treatment of allergic diseases" provocation tests are accepted as primary outcomes for dose-finding studies.

For the CPT increasing doses of Phleum pollen solutions are applied to the eye and characteristic symptoms (eye redness, weeping, itching or burning, and nose dripping/blockage) are assessed at each concentration: 0=absent, 1=mild, 2=moderate, 3=severe. At a score value of >=5/concentration the test is considered positive and finished.

It is expected that at the end of the study higher doses are necessary to provoke a positive CPT.

Furthermore comparative evaluation of the safety data (AEs) in the different dosage groups is a very important parameter for the evaluation of the outcome of the study.

Enrollment

308 patients

Sex

All

Ages

18 to 70 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

appropriately signed and dated ICON prior to study specific action
IgE-mediated Sensitization against grass pollen
Perception of disease activity of at least 30 mm on a 100 mm VAS
FEV1 or a PEFR value > 80% of predicted normal value
Allergic rhinitis and/or rhinoconjunctivitis symptoms (at least 2 years) with or without intermittent asthma symptoms verified by:
- suggestive medical history AND
- specific IgE against grass pollen with CAP-RAST ≥ 2 AND
- a positive SPT (wheal diameter ≥ 3 mm) AND
- a positive CPT for grass pollen
Patients with co-allergies are allowed to enter the study:
- being asymptomatic against co-allergens such as tree or weed pollen, house dust mites, cat and dog, and other country specific allergens
- with CAP-RAST co-allergen < grass (detailed specifications given for Birch, HDM, animal dander, other country specific allergens)
- All other co-allergens: difference in CAP RAST co-allergen to grass of ≥ 2 and an SPT wheal diameter co-allergen < grass
Females of non-childbearing potential must be postmenopausal for at least

1 year or surgically sterilized
Females of childbearing potential must be non-lactating, non-pregnant and must correctly use an effective method of contraception during the study.

Exclusion criteria

Acute or chronic infectious conjunctivitis
History of significant clinical manifestations of allergy as a result of sensitisation against trees or weed pollen and perennial allergens (e.g., house dust mites)

Patients are not allowed to enter into the study:

with typical symptoms against co-allergens such as tree or weed pollen, HDM, cat and dog, and other country specific allergens
with CAP-RAST co-allergen ≥ grass
- Persistent asthma, according to Global Initiative for Asthma (GINA)
- Acute or chronic inflammatory or infectious airways disease
- Chronic structural disease of the lung (e.g., emphysema or bronchiectasis)
- Autoimmune and/or immune deficiency
- Any disease that prohibits the use of adrenaline (e.g., hyperthyroidism)
- Severe uncontrolled disease that could increase the risk to the patients while participating in the study, including but not limited to: cardiovascular insufficiency, severe or unstable lung diseases, endocrine diseases, clinically significant renal or hepatic diseases or haematological disorders.
- Active malignant disease during the previous 5 years
- Significant abnormal laboratory parameter or alteration in vital signs that could increase the risk to the study patient
- Abuse of alcohol, drugs or medications within the past year
- Severe psychiatric, psychological or neurological disorder
- Immunotherapy against grass pollen within the last 5 years
- Systemic and/or topical treatment with β-blockers within 1 wk prior to V2
- Use of medication that may interfere with the immune system or has been using any medication which might still have an influence on the immune system at V2
- Use of tranquiliser or psychoactive drugs within 1 week prior to V1
- Use of systemic corticosteroids within 3 months prior to V1
- Immunization with vaccines within 7 days prior to V2
- Expected non-compliance and/or no cooperation
- Participation in another clinical study within 30 days prior to V2
- Prior participation in this study
- Employees at the investigational centre or first degree relative or partner of the investigator
- Planed donation of germ cells, blood, organs or bone marrow during the course of the study
- Contractually not capable
- A positive pregnancy test at V1
- Jurisdictional or governmentally institutionalised.