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Privileged Antigen Presentation in Splenic B Cell Follicles Maximizes T Cell Responses in Prime-Boost Vaccination
Author(s) -
Byram W. Bridle,
Andrew Nguyen,
Omar Salem,
Liang Zhang,
Sandeep T. Koshy,
Derek L. Clouthier,
Lan Chen,
Jonathan Pol,
Stephanie L. Swift,
Dawn M. E. Bowdish,
Brian D. Lichty,
Jonathan L. Bramson,
Yonghong Wan
Publication year - 2016
Publication title -
the journal of immunology
Language(s) - Uncategorized
Resource type - Journals
SCImago Journal Rank - 2.737
H-Index - 372
eISSN - 1550-6606
pISSN - 0022-1767
DOI - 10.4049/jimmunol.1600106
Subject(s) - cd11c , immunology , cytotoxic t cell , antigen presenting cell , cd8 , antigen presentation , biology , spleen , effector , antigen , microbiology and biotechnology , t cell , immune system , in vitro , phenotype , biochemistry , gene
Effector T cells (TEFF) are a barrier to booster vaccination because they can rapidly kill Ag-bearing APCs before memory T cells are engaged. We report in this study that i.v. delivery of rhabdoviral vectors leads to direct infection of follicular B cells in the spleen, where the earliest evidence of secondary T cell responses was observed. This allows booster immunizations to rapidly expand CD8(+) central memory T cells (TCM) during the acute phase of the primary response that is dominated by TEFF Interestingly, although the ablation of B cells before boosting with rhabdoviral vectors diminishes the expansion of memory T cells, B cells do not present Ags directly. Instead, depletion of CD11c(+) dendritic cells abrogates secondary T cell expansion, suggesting that virus-infected follicular B cells may function as an Ag source for local DCs to subsequently capture and present the Ag. Because TCM are located within B cell follicles in the spleen whereas TEFF cannot traffic through follicular regions, Ag production and presentation by follicular APCs represent a unique mechanism to secure engagement of TCM during an ongoing effector response. Our data offer insights into novel strategies for rapid expansion of CD8(+) T cells using prime-boost vaccines by targeting privileged sites for Ag presentation.

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