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Evaluation of Nasal Mucosal Permeability in Controls and House Dust Mite Allergic Rhinitis Patients

U

Universitaire Ziekenhuizen KU Leuven

Status

Completed

Conditions

Allergic Rhinitis

Treatments

Other: AR patients without medication
Other: healthy controls
Other: AR patients with use of nasal corticoid spray

Study type

Interventional

Funder types

Other

Identifiers

NCT02461797
biopsystudy

Details and patient eligibility

About

Recently, a critical role in the development of allergic rhinitis (AR) has been attributed to the nasal epithelium. The airway epithelium forms a physical barrier, protecting the nasal mucosa and underlying organs from damage from contact with exogenous particles. The nasal epithelial barrier is primarily determined by the integrity of the airway epithelium, in which epithelial cells are connected to each other by complex network structures like tight junctions (TJs), ultimately sealing off the paracellular space. TJs consist of different transmembrane proteins including occludin, tricellulin, the claudin family, and junctional adhesion molecules. TJ form intercellular homodimers/heterodimers between neighboring cells. Scaffold adaptor proteins like cingulin and the zonula occludens family connect the transmembrane proteins to the actin cytoskeleton.

Disturbed TJ function can facilitate the entrance of foreign pathogens and antigens into the submucosal layer, giving raise to allergic sensitization via increased access of allergens to the dendritic cells and/or inducing persistent inflammation via activation of mast cells and other inflammatory cells residing in the upper airways. Chronic disorders like allergic asthma, inflammatory bowel disease and atopic dermatitis have been linked to defective or altered TJ function. Recently, an impaired epithelial barrier function was found in patients with chronic rhinosinusitis with nasal polyps (CRSwNP), suggesting changes in TJ arrangement in the nasal cavity. CRSwNP presents a similar inflammation of the sinonasal cavities as found in AR patients, i.e. a Th2 cytokine driven inflammation with tissue eosinophilia. Nevertheless, the role of TJs and its regulation has not been investigated in AR.

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Enrollment

26 patients

Sex

All

Ages

18 to 60 years old

Volunteers

Accepts Healthy Volunteers

Inclusion criteria

  1. Patients with an ARIA-based diagnosis of persistent moderate/severe AR (≥ 2 nasal symptoms suggestive of allergic rhinitis and positive skin prick tests to HDM (HAL Allergy, Leiden, The Netherlands), and with VAS score for total nasal symptoms of more than 5
  2. Age > 18 and < 60 years.
  3. Possibility to give reliable information and written informed consent
  4. For AR group with nasal corticosteroid spray: Patients that use nasal corticosteroid spray for at least three weeks prior to the study, with a minimum application of two puffs per nostril once a day.

Exclusion criteria

  1. No common cold in the last 4 weeks

  2. Patients on prolonged use of decongestive nose sprays, suffering from so-called rhinitis medicamentosa

  3. A. For healthy controls and AR without use of nasal spray: Patients using other nasal or oral medication affecting nasal function, like nasal corticosteroids, anticholinergics, cromoglycates, leukotriene antagonists, ACE inhibitors less than 4 weeks before start of the study.

    B. For AR group with use of nasal corticosteroid spray: Patients using other nasal or oral medication affecting nasal function, like anticholinergics, cromoglycates, leukotriene antagonists, ACE inhibitors less than 4 weeks before start of the study.

  4. Nasal endoscopic evidence of rhinosinusitis w/wo NP or structural abnormalities such as clinically relevant septal deviation (septum reaching concha inferior or lateral nasal wall) or septal perforation

  5. Patients on immunotherapy (IT) for house dust mite (HDM) or with history of IT for HDM

  6. Patient with a psychiatric, addictive, or any disorder of which the investigators feel that this may compromise the ability to give truly informed consent for participation in this study or provide reliable information on the questionnaire

  7. Patients being enrolled in other clinical trials

  8. Pregnancy or breastfeeding

  9. Malignancies or severe comorbidity

  10. Contra-indication for local anesthesia with cocaine 5%

  11. Smoking

  12. Use of anticoagulation medication

Healthy controls will meet the same exclusion criteria, with additional inclusion criteria:

  1. Absence of nasal symptoms
  2. Negative history of respiratory allergy
  3. Negative skin prick test (SPT) results

Trial design

Primary purpose

Basic Science

Allocation

Non-Randomized

Interventional model

Parallel Assignment

Masking

None (Open label)

26 participants in 3 patient groups

healthy controls
Other group
Description:
biopsy of nasal mucosa healthy controls
Treatment:
Other: healthy controls
AR patients with use of nasal corticoid spray
Other group
Description:
biopsy of nasal mucosa allergic rhinitis to house dust mite with nasal corticosteroid spray
Treatment:
Other: AR patients with use of nasal corticoid spray
AR patients without medication
Other group
Description:
biopsy of nasal mucosa allergic rhinitis to house dust mite without any use of medication for symptom control
Treatment:
Other: AR patients without medication

Trial contacts and locations

1

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Data sourced from clinicaltrials.gov

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