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Intradermal Allergen Immunotherapy for Allergic Rhinitis: Current Evidence.

Kawita AtipasDichapong KanjanawaseePongsakorn Tantilipikorn
Published in: Journal of personalized medicine (2022)
Allergic rhinitis (AR) is an immunoglobulin E (IgE)-mediated inflammatory disease that is induced by allergen introduction to the nasal mucosa, which triggers an inflammatory response. The current treatments for AR include allergen avoidance and pharmacotherapy; however, allergen-specific immunotherapy (AIT) is the only treatment that can be employed to modify immunologic responses and to achieve a cure for allergic diseases. The current standard routes of AIT administration are the subcutaneous and sublingual routes. Alternatively, the dermis contains a high density of dermal dendritic cells that act as antigen-presenting cells, so intradermal administration may confer added advantages and increase the efficacy of AIT. Moreover, intradermal immunotherapy (IDIT) may facilitate a reduction in the allergen dosage and a shortening of the treatment duration. The aim of this review was to search and evaluate the current evidence specific to IDIT, including its modified formulations, such as allergoids and peptides. The results of this review reveal conflicting evidence that suggests that the overall benefit of IDIT remains unclear. As such, further clinical trials are needed to establish the clinical utility of IDIT, and to determine the optimal treatment-related protocols.
Keyphrases
  • allergic rhinitis
  • inflammatory response
  • clinical trial
  • dendritic cells
  • oxidative stress
  • dna methylation
  • genome wide
  • combination therapy
  • cell death
  • smoking cessation
  • single cell
  • lps induced
  • phase iii