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A mucosal vaccine against Chlamydia trachomatis generates two waves of protective memory T cells
Authors
David Alvarez
P. A. Basto
+13 more
Omid Cameron Farokhzad
D. Gondek
Robert S. Langer
A Olive
M. Perro
A. F. Radovic-Moreno
Jinjun Shi
Michael N. Starnbach
G Stary
Andrew Martin Tager
Ulrich H. von Andrian
V. D. Vrbanac
J. A. Yethon
Publication date
20 October 2016
Publisher
'American Association for the Advancement of Science (AAAS)'
Doi
Abstract
Genital Chlamydia trachomatis (Ct) infection induces protective immunity that depends on interferon-γ producing CD4 T-cells. By contrast, mucosal exposure to ultraviolet light (UV)-inactivated Ct (UV-Ct) generated regulatory T-cells that exacerbated subsequent Ct infection. We show that mucosal immunization with UV-Ct complexed with charge-switching synthetic adjuvant particles (cSAP) elicited long-lived protection in conventional and humanized mice. UV-Ct-cSAP targeted immunogenic uterine CD11b+CD103− dendritic cells (DCs), whereas UV-Ct accumulated in tolerogenic CD11b−CD103+ DCs. Regardless of vaccination route, UV-Ct-cSAP induced systemic memory T-cells, but only mucosal vaccination induced effector T-cells that rapidly seeded uterine mucosa with resident memory T-cells (TRM). Optimal Ct clearance required both TRM seeding and subsequent infection-induced recruitment of circulating memory T-cells. Thus, UV-Ct-cSAP vaccination generated two synergistic memory T-cell subsets with distinct migratory properties
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Harvard University - DASH
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Last time updated on 17/04/2018