Birbeck Granules Are Subdomains of Endosomal Recycling Compartment in Human Epidermal Langerhans Cells, Which Form Where Langerin Accumulates

  1. Daniel Hanau#
  1. Unité Mixte de Recherche 144 Centre National de laRecherche Scientifique-Institut Curie, *Laboratoire Mécanismes Moléculaires du Transport Intracellulaire and
  2. Laboratoire de Microscopie Electronique, Institut Curie, 75248 Paris, France;
  3. Institut National de la Santéet de la Recherche Médicale EP 99–08 Biologie des Cellules Dendritiques Humaines and
  4. Institut National de la Santé et de la Recherche Médicale U 311, Etablissement Français du Sang-Alsace, 67065 Strasbourg, France; and
  5. §Department of Dermatology and Center for Electron Microscopy, Leidem University Medical Center, 2300 RA Leiden, The Netherlands
  1. Suzanne R. Pfeffer, Monitoring Editor
  • Submitted June 20, 2001.
  • Revised October 11, 2001.
  • Accepted October 31, 2001.

Abstract

Birbeck granules are unusual rod-shaped structures specific to epidermal Langerhans cells, whose origin and function remain undetermined. We investigated the intracellular location and fate of Langerin, a protein implicated in Birbeck granule biogenesis, in human epidermal Langerhans cells. In the steady state, Langerin is predominantly found in the endosomal recycling compartment and in Birbeck granules. Langerin internalizes by classical receptor-mediated endocytosis and the first Birbeck granules accessible to endocytosed Langerin are those connected to recycling endosomes in the pericentriolar area, where Langerin accumulates. Drug-induced inhibition of endocytosis results in the appearance of abundant open-ended Birbeck granule-like structures appended to the plasma membrane, whereas inhibition of recycling induces Birbeck granules to merge with a tubular endosomal network. In mature Langerhans cells, Langerin traffic is abolished and the loss of internal Langerin is associated with a concomitant depletion of Birbeck granules. Our results demonstrate an exchange of Langerin between early endosomal compartments and the plasma membrane, with dynamic retention in the endosomal recycling compartment. They show that Birbeck granules are not endocytotic structures, rather they are subdomains of the endosomal recycling compartment that form where Langerin accumulates. Finally, our results implicate ADP-ribosylation factor proteins in Langerin trafficking and the exchange between Birbeck granules and other endosomal membranes.

Footnotes

  • These authors contributed equally to this work and are listed in alphabetical order.

  • # Corresponding author. E-mail address:daniel.hanau{at}efs-alsace.fr.

  • Article published online ahead of print. Mol. Biol. Cell 10.1091/mbc.01–06-0300. Article and publication date are atwww.molbiolcell.org/cgi/doi/10.1091/mbc.01–06-0300.

  • Abbreviations used:

    Au
    gold-labeled
    BG
    Birbeck granule
    ERC
    endosomal recycling compartment
    Fi
    freshly isolated
    LC
    Langerhans cell
    TGN
    trans-Golgi network
    • | Table of Contents

    This Article

    1. Published online before print December 7, 2001, doi: 10.1091/mbc.01-06-0300 Mol. Biol. Cell vol. 13 no. 1 317-335
    1. » Abstract
    2. Full Text
    3. Full Text (PDF)
    4. PDF + Supp Data
    5. MBC Notice
    6. All Versions of this Article:
      1. 01-06-0300v1
      2. 01-06-0300v2
      3. 13/1/317 most recent

    Classifications

    Article Usage Stats

    1. Article Usage Statistics

    Current Issue

    1. July 15, 2017, 28 (15)
    1. Current Issue
    1. Alert me to new issues of Mol. Biol. Cell

    Most