A toll-like receptor 2/6-agonist prevents allergic airway inflammation in chronic respiratory sensitisation

Background: The hygiene hypothesis negatively correlates the microbial burden of the environment to the prevalence of Th2-related disorders, e.g. allergy and asthma. This is explained by a Th1-triggering through pathogen-associated patterns sensed via toll-like receptors. Objective: To discover mechanisms which prevent the development of chronic allergic inflammation. Methods: In a chronic model of allergic airway inflammation induced by intranasal Timothy grass pollen allergen extract administrations, early-onset toll-like receptor agonisation and/or interferon-a~ administration was compared to the therapeutic and immune-modulating effects of dexamethasone. Results: By toll-like receptor 2/6-agonisation allergic inflammation and airway remodelling were reduced. Lymphocyte counts were not changed, nor did the cytokine profile or the number of CD41foxp31cells in draining lymph nodes prove a Th2/Th1-shift or the induction of tolerance. Dexamethasone reduced both sensitisation as well as allergic inflammation, and, moreover, CD11c1cells in lymph nodes. Stimulation experiments point to a general unresponsiveness of splenocytes after toll-like receptor agonisation, implicating a T-cell anergy. Conclusion: The toll-like receptor 2/6-agonist is a promising preventive approach in diseases related to exaggerated T-cell responses, e.g., allergy, and asthma.