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Pulmonary delivery of DNA vaccine constructs using deacylated PEI elicits immune responses and protects against viral challenge infection.

J Control Release.. 2013-09; 
Mann JF, McKay PF, Arokiasamy S, Patel RK, Klein K, Shattock RJ. a Imperial College London, Department of Infectious Diseases, Division of Medicine, Norfolk Place, London W2 1PG, UKb Centre for Infection and Immunity, Division of Clinical Sciences, St Georges University of London, London SW17 0RE, UK
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摘要

Vaccination through mucosal surfaces has been shown to elicit antiviral immune responses against a number of mucosal pathogens. Here we demonstrate that both mucosal and systemic immune responses can be elicited against a model HIV-1 CN54gp140 antigen when cation-complexed plasmid DNA vaccines are applied topically to the murine pulmonary mucosa as an immune priming strategy. Furthermore, using an influenza challenge model we show that a plasmid DNA vaccine complexed to a less toxic form of PEI called dPEI (a nearly fully hydrolysed linear PEI with 11% additional free protonatable nitrogen atoms) can provide significant protection against a respiratory challenge infection in mice. Furthermore, we show that dPEI... More

关键词

Mucosal; Vaccination; Gene delivery; Immunity; HIV-1; Influenza