Research
Chitosan IFN-γ-pDNA Nanoparticle (CIN) Therapy for Allergic Asthma
-
* Corresponding author: Shyam S Mohapatra smohapat@hsc.usf.edu
The Joy McCann Culverhouse Airway Disease Center, Division of Allergy and Immunology, University of South Florida College of Medicine and James A Haley VA Hospital, Tampa, FL, USA
Genetic Vaccines and Therapy 2003, 1:3 doi:10.1186/1479-0556-1-3
Published: 27 October 2003Abstract
Background
Allergic subjects produce relatively low amounts of IFN-γ, a pleiotropic Th-1 cytokine that downregulates Th2-associated airway inflammation and hyperresponsiveness (AHR), the hallmarks of allergic asthma. Adenovirus-mediated IFN-γ gene transfer reduces AHR, Th2 cytokine levels and lung inflammation in mice, but its use would be limited by the frequency of gene delivery required; therefore, we tested chitosan/IFN-γ pDNA nanoparticles (CIN) for in situ production of IFN-γ and its in vivo effects.
Methods
CIN were administered to OVA-sensitized mice to investigate the possibility of using gene transfer to modulate ovalbumin (OVA)-induced inflammation and AHR.
Results
Mice treated with CIN exhibit significantly lower AHR to methacholine challenge and less lung histopathology. Production of IFN-γ is increased after CIN treatment while the Th2-cytokines, IL-4 and IL-5, and OVA-specific serum IgE are reduced compared to control mice. AHR and eosinophilia are also significantly reduced by CIN therapy administered therapeutically in mice with established asthma. CIN was found to inhibit epithelial inflammation within 6 hours of delivery by inducing apoptosis of goblet cells. Experiments performed on STAT4-defective mice do not show reduction in AHR with CIN treatment, thus implicating STAT4 signaling in the mechanism of CIN action.
Conclusion
These results demonstrate that mucosal CIN therapy can effectively reduce established allergen-induced airway inflammation and AHR.