| Literature DB >> 27595442 |
John P Graham1, Pierre Authie1, Chun I Yu1, Sandra M Zurawski2, Xiao-Hua Li2, Florentina Marches3, Anne-Laure Flamar2, Aditi Acharya2, Jacques Banchereau4, A Karolina Palucka5.
Abstract
The targeting of vaccine antigens to antigen presenting cells (APC), such as dendritic cells (DCs), is a promising strategy for boosting vaccine immunogenicity and, in turn, protective and/or therapeutic efficacy. However, in vivo systems are needed to evaluate the potential of this approach for testing human vaccines. To this end, we examined human CD8(+) T-cell expansion to novel DC-targeting vaccines in vitro and in vivo in humanized mice. Vaccines incorporating the influenza matrix protein-1 (FluM1) antigen fused to human specific antibodies targeting different DC receptors, including DEC-205, DCIR, Dectin-1, and CD40, elicited human CD8(+) T-cell responses, as defined by the magnitude of specific CD8(+) T-cells to the targeted antigen. In vitro we observed differences in response to the different vaccines, particularly between the weakly immunogenic DEC-205-targeted and more strongly immunogenic CD40-targeted vaccines, consistent with previous studies. However, in humanized mice adoptively transferred (AT) with mature human T cells (HM-T), vaccines that performed weakly in vitro (i.e., DEC-205, DCIR, and Dectin-1) gave stronger responses in vivo, some resembling those of the strongly immunogenic CD40-targeted vaccine. These results demonstrate the utility of the humanized mouse model as a platform for studies of human vaccines.Entities:
Keywords: Cytotoxic T cells; Dendritic cell targeted vaccines; Human dendritic cells; Humanized mice
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Year: 2016 PMID: 27595442 PMCID: PMC5598757 DOI: 10.1016/j.vaccine.2016.08.071
Source DB: PubMed Journal: Vaccine ISSN: 0264-410X Impact factor: 3.641