| Literature DB >> 26682983 |
Andrés Alloatti1, Fiorella Kotsias2, Anne-Marie Pauwels3, Jean-Marie Carpier1, Mabel Jouve4, Evy Timmerman5, Luigia Pace1, Pablo Vargas6, Mathieu Maurin1, Ulf Gehrmann1, Leonel Joannas1, Omar I Vivar1, Ana-Maria Lennon-Duménil1, Ariel Savina7, Kris Gevaert5, Rudi Beyaert3, Eik Hoffmann8, Sebastian Amigorena9.
Abstract
The initiation of cytotoxic immune responses by dendritic cells (DCs) requires the presentation of antigenic peptides derived from phagocytosed microbes and infected or dead cells to CD8(+) T cells, a process called cross-presentation. Antigen cross-presentation by non-activated DCs, however, is not sufficient for the effective induction of immune responses. Additionally, DCs need to be activated through innate receptors, like Toll-like receptors (TLRs). During DC maturation, cross-presentation efficiency is first upregulated and then turned off. Here we show that during this transient phase of enhanced cross-presentation, phago-lysosome fusion was blocked by the topological re-organization of lysosomes into perinuclear clusters. LPS-induced lysosomal clustering, inhibition of phago-lysosome fusion and enhanced cross-presentation, all required expression of the GTPase Rab34. We conclude that TLR4 engagement induces a Rab34-dependent re-organization of lysosomal distribution that delays antigen degradation to transiently enhance cross-presentation, thereby optimizing the priming of CD8(+) T cell responses against pathogens.Entities:
Keywords: GTPase Rab34; Toll-like receptor 4; antigen presentation; cross-presentation; dendritic cell; phagocytosis; phagosome maturation
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Year: 2015 PMID: 26682983 DOI: 10.1016/j.immuni.2015.11.006
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745