1. Langerin-mediated internalization of a modified peptide routes antigens to early endosomes and enhances cross-presentation by human Langerhans cells.
- Author
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Fehres CM, Duinkerken S, Bruijns SC, Kalay H, van Vliet SJ, Ambrosini M, de Gruijl TD, Unger WW, Garcia-Vallejo JJ, and van Kooyk Y
- Subjects
- Antibodies metabolism, Cell Compartmentation, Cell Differentiation drug effects, Cross-Priming drug effects, Endosomes drug effects, Humans, Langerhans Cells cytology, Langerhans Cells drug effects, Ligands, Poly I-C pharmacology, Skin metabolism, Toll-Like Receptors metabolism, Antigens metabolism, Antigens, CD metabolism, Cross-Priming immunology, Endocytosis drug effects, Endosomes metabolism, Langerhans Cells metabolism, Lectins, C-Type metabolism, Mannose-Binding Lectins metabolism, Peptides metabolism
- Abstract
The potential of the skin immune system to generate immune responses is well established, and the skin is actively exploited as a vaccination site. Human skin contains several antigen-presenting cell subsets with specialized functions. In particular, the capacity to cross-present exogenous antigens to CD8+ T cells is of interest for the design of effective immunotherapies against viruses or cancer. Here, we show that primary human Langerhans cells (LCs) were able to cross-present a synthetic long peptide (SLP) to CD8
+ T cells. In addition, modification of this SLP using antibodies against the receptor langerin, but not dectin-1, further enhanced the cross-presenting capacity of LCs through routing of internalized antigens to less proteolytic early endosome antigen 1+ early endosomes. The potency of LCs to enhance CD8+ T-cell responses could be further increased through activation of LCs with the toll-like receptor 3 ligand polyinosinic:polycytidylic acid (pI:C). Altogether, the data provide evidence that human LCs are able to cross-present antigens after langerin-mediated internalization. Furthermore, the potential for antigen modification to target LCs specifically provides a rationale for generating effective anti-tumor or anti-viral cytotoxic T lymphocyte responses.- Published
- 2017
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