PLoS ONE (Jan 2014)

Dendritic cells utilize the evolutionarily conserved WASH and retromer complexes to promote MHCII recycling and helper T cell priming.

  • Daniel B Graham,
  • Douglas G Osborne,
  • Joshua T Piotrowski,
  • Timothy S Gomez,
  • Grzegorz B Gmyrek,
  • Holly M Akilesh,
  • Adish Dani,
  • Daniel D Billadeau,
  • Wojciech Swat

DOI
https://doi.org/10.1371/journal.pone.0098606
Journal volume & issue
Vol. 9, no. 6
p. e98606

Abstract

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Immature dendritic cells (DCs) maintain a highly dynamic pool of recycling MHCII that promotes sampling of environmental antigens for presentation to T helper cells. However, the molecular basis of MHCII recycling and the cellular machinery that orchestrates MHCII trafficking are incompletely understood. Using a mouse model we show that WASH, an actin regulatory protein that facilitates retromer function, is essential for MHCII recycling and efficient priming of T helper cells. We further demonstrate that WASH deficiency results in impaired MHCII surface levels, recycling, and an accumulation of polyubiquitinated MHCII complexes, which are subsequently slated for premature lysosomal degradation. Consequently, conditional deletion of the Wash gene in DCs impairs priming of both conventional and autoimmune T helper cells in vivo and attenuates disease progression in a model of experimental autoimmune encephalitis (EAE). Thus, we identify a novel mechanism in which DCs employ the evolutionarily conserved WASH and retromer complex for MHCII recycling in order to regulate T helper cell priming.