Frontiers in Immunology (Jul 2024)

Intranasal administration of a synthetic TLR4 agonist INI-2004 significantly reduces allergy symptoms following therapeutic administration in a murine model of allergic sensitization

  • Konner J. Jackson,
  • Cassandra Buhl,
  • Shannon M. Miller,
  • Juhienah K. Khalaf,
  • Janine Ward,
  • Cherrokee Sands,
  • Lois Walsh,
  • Margaret Whitacre,
  • David J. Burkhart,
  • Hélène G. Bazin-Lee,
  • Jay T. Evans

DOI
https://doi.org/10.3389/fimmu.2024.1421758
Journal volume & issue
Vol. 15

Abstract

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IntroductionAtopic diseases have been steadily increasing over the past decades and effective disease-modifying treatment options are urgently needed. These studies introduce a novel synthetic Toll-like receptor 4 (TLR4) agonist, INI-2004, with remarkable efficacy as a therapeutic intranasal treatment for seasonal allergic rhinitis.MethodsUsing a murine airway allergic sensitization model, the impact of INI-2004 on allergic responses was assessed.ResultsOne or two intranasal doses of INI-2004 significantly reduced airway resistance, eosinophil influx, and Th2 cytokine production – providing strong evidence of allergic desensitization. Further investigations revealed that a liposomal formulation of INI-2004 exhibited better safety and efficacy profiles compared to aqueous formulations. Importantly, the liposomal formulation demonstrated a 1000-fold increase in the maximum tolerated intravenous dose in pigs. Pre-clinical GLP toxicology studies in rats and pigs confirmed the safety of liposomal INI-2004, supporting its selection for human clinical trials.DiscussionThese findings lay the groundwork for the ongoing clinical evaluation of INI-2004 in allergic rhinitis as a stand-alone therapy for individuals poly-sensitized to multiple seasonal allergens. The study underscores the significance of innovative immunotherapy approaches in reshaping the landscape of allergic rhinitis management.

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