Molecular and Cellular Mechanism in the Course of Immunotherapy With a Phleum Pratense Oral Lyophilisate

ALK-Abelló

Status and phase

Completed

Phase 4

Conditions

Allergic Rhinitis Due to Grass Pollens

Treatments

Drug: Grazax

Other: Placebo

Study type

Interventional

Funder types

Industry

Identifiers

NCT01854736

GT-24

2012-005092-14 (EudraCT Number)

Details and patient eligibility

About

This trial is an exploratory randomised, parallel-group, double-blind, placebo- controlled, national, single-centre trial.

The trial will be initiated before 2013 grass pollen season and subjects will be randomised in September 2013 to receive active treatment (Grazax®) or placebo during 2 years. Placebo group will be treated 2 years with placebo and a third year with active therapy (Grazax®) and active group will continue the active treatment in the third year. In the last year, all placebo patients will be changed to active group and active and placebo patients will be informed about, but the trial will not be unblinded until the end of the third year and patients won´t know what treatment they were assigned to during the first 2 years.

Full description

There is a first stage of clinical trial (GT-20) in which ALK- Abelló is directly working into the MEICA project to explore human immunological mechanisms of SIT (observed after Grazax® treatment). In this trial, different potential biomarkers of early and sustained effect of specific immunotherapy have been identified. Therefore, for a further research, it was necessary to carry on a new clinical double blind placebo control trial to evaluate a selected panel of biomarkers that can be applied in the selection and monitoring of patients during immunotherapy. They can be of value in the evaluation of future product candidates for specific immunotherapy. For this purpose, it is necessary that the Biomarkers selected, clearly differentiate between active and placebo treated groups. Moreover, specific immunological changes differences between active and placebo patients during pollen seasons are unknown. This first study allowed us identifying a potential set of biomarkers and time points for each of them that might correlate with treatment effect. This second study is needed to evaluate the potential of these biomarkers to discriminate placebo treated patients and it is a necessary step before incorporating them in big prospective efficacy studies.

A third year in an active IMP design after the two years in a double blind placebo setup is included as a way to validate the differences observed intergroup during the first year of therapy. This is needed as pollen seasons significantly differ in strength and duration. Moreover, there is a unique opportunity of analysing immunological changes of the intervention before a careful baseline monitoring of patients undergoing placebo treatment, with the opportunity of understanding immunological clues in the natural evolution of allergy disease.

Enrollment

51 patients

Sex

All

Ages

18 to 65 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

A history of grass pollen allergy
Positive skin prick test to grass
Positive specific IgE against Phl p 5
Written informed consent before entering the trial.
Female subjects who are fertile must have a negative pregnancy test and be willing to practise appropriate contraceptive methods.
Subject willing and able to comply with the trial protocol.

Exclusion criteria

Previous treatment by immunotherapy with grass allergen extracts.
Ongoing treatment with any allergen specific immunotherapy product.
Previous or ongoing treatment with Omalizumab, mono amine oxidase (MAO) inhibitors or tricyclic antidepressant medication.
Use of medication at the screening visit which can interfere with SPT results
A clinical history of symptomatic perennial allergic rhinitis or asthma.
History of allergy, hypersensitivity or intolerance to the excipients of IMP (except for Phleum pratense).
Systemic disease affecting the immune system (e.g. autoimmune disease, immune complex disease, or immune deficiency disease).
Any clinically relevant chronic disease (≥ 3 months duration) (e.g. cystic fibrosis, malignancy, type I diabetes mellitus, malabsorption or malnutrition, renal or hepatic insufficiency).
Inflammatory conditions in the oral cavity with severe symptoms such as oral lichen planus with ulcerations or severe oral mycosis at randomisation.
FEV1 ≤ 70% of predicted value.
Symptoms of or treatment for upper respiratory tract infection, acute sinusitis, acute otitis media or other relevant infectious process at randomisation.
Being immediate family of the investigator or trial staff.
A mental condition rendering the subject unable to understand the nature, scope and possible consequences of the trial, and/or evidence of an uncooperative attitude.
Unlikely to be able to complete the trial, for any reason, or likely to move, or travel for extended periods of time during the trial period.
Use of an investigational drug within 30 days or 5 half-lives, whichever is longest, prior to screening.