Disruption of the langerin / CD207 Gene Abolishes Birbeck Granules without a Marked Loss of Langerhans Cell Function

Author:

Kissenpfennig Adrien1,Aït-Yahia Smina2,Clair-Moninot Valérie2,Stössel Hella3,Badell Edgar4,Bordat Yann4,Pooley Joanne L.5,Lang Thierry6,Prina Eric6,Coste Isabelle2,Gresser Olivia1,Renno Toufic2,Winter Nathalie4,Milon Geneviève6,Shortman Ken5,Romani Nikolaus3,Lebecque Serge2,Malissen Bernard1,Saeland Sem2,Douillard Patrice2

Affiliation:

1. Centre d'Immunologie de Marseille-Luminy, INSERM-CNRS-Université de la Méditerranée, Parc Scientifique de Luminy, Marseille

2. Laboratory for Immunological Research, Schering Plough, Dardilly

3. Department of Dermatology, Innsbruck Medical University, Innsbruck, Austria

4. Unité de Génétique Mycobactérienne, Institut Pasteur, Paris, France

5. The Walter and Eliza Hall Institute of Medical Research, Victoria, Australia

6. Unité d'Immunophysiologie et Parasitisme Intracellulaire

Abstract

ABSTRACT Langerin is a C-type lectin expressed by a subset of dendritic leukocytes, the Langerhans cells (LC). Langerin is a cell surface receptor that induces the formation of an LC-specific organelle, the Birbeck granule (BG). We generated a langerin / mouse on a C57BL/6 background which did not display any macroscopic aberrant development. In the absence of langerin, LC were detected in normal numbers in the epidermis but the cells lacked BG. LC of langerin / mice did not present other phenotypic alterations compared to wild-type littermates. Functionally, the langerin / LC were able to capture antigen, to migrate towards skin draining lymph nodes, and to undergo phenotypic maturation. In addition, langerin / mice were not impaired in their capacity to process native OVA protein for I - A b -restricted presentation to CD4 + T lymphocytes or for H - 2K b -restricted cross-presentation to CD8 + T lymphocytes. langerin / mice inoculated with mannosylated or skin-tropic microorganisms did not display an altered pathogen susceptibility. Finally, chemical mutagenesis resulted in a similar rate of skin tumor development in langerin / and wild-type mice. Overall, our data indicate that langerin and BG are dispensable for a number of LC functions. The langerin / C57BL/6 mouse should be a valuable model for further functional exploration of langerin and the role of BG.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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