Induction of mucosal immune responses against <i>Helicobacter pylori</i> infection after sublingual and intragastric route of immunization

Louise Sjökvist Ottsjö(University of Gothenburg), Frida Jeverstam(University of Gothenburg), Linda Yrlid(University of Gothenburg), Alexander U. Wenzel(University of Gothenburg), Anna K. Walduck(RMIT University), Sukanya Raghavan(University of Gothenburg)
Immunology
September 27, 2016
Cited by 28Open Access
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Abstract

Summary There is a current lack of effective mucosal vaccines against major gastroenteric pathogens and particularly against Helicobacter pylori , which causes a chronic infection that can lead to peptic ulcers and gastric cancer in a subpopulation of infected individuals. Mucosal CD 4 + T‐cell responses have been shown to be essential for vaccine‐induced protection against H. pylori infection. The current study addresses the influence of the adjuvant and site of mucosal immunization on early CD 4 + T‐cell priming to H. pylori antigens. The vaccine formulation consisted of H. pylori lysate antigens and mucosal adjuvants, cholera toxin ( CT ) or a detoxified double‐mutant heat‐labile enterotoxin from Escherichia coli (dm LT ), which were administered by either the sublingual or intragastric route. We report that in vitro , adjuvants CT and dm LT induce up‐regulation of pro‐inflammatory gene expression in purified dendritic cells and enhance the H. pylori ‐specific CD 4 + T‐cell response including interleukin‐17A ( IL ‐17A), interferon‐ γ ( IFN ‐ γ ) and tumour necrosis factor‐ α ( TNF ‐ α ) secretion. In vivo , sublingual immunization led to an increased frequency of IL ‐17A + , IFN ‐ γ + and TNF ‐ α + secreting CD 4 + T cells in the cervical lymph nodes compared with in the mesenteric lymph nodes after intragastric immunization. Subsequently, IL ‐17A + cells were visualized in the stomach of sublingually immunized and challenged mice. In summary, our results suggest that addition of an adjuvant to the vaccine clearly activated dendritic cells, which in turn, enhanced CD 4 + T‐cell cytokines IL ‐17A, IFN ‐ γ and TNF ‐ α responses, particularly in the cervical lymph nodes after sublingual vaccination.


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