IRAP Identifies an Endosomal Compartment Required for MHC Class I Cross-Presentation

Loredana Saveanu; Oliver Carroll; Mirjana Weimershaus; Pierre Guermonprez; Elke Firat; Viv Lindo; Fiona Greer; Jean Davoust; Roland Kratzer; Susanna R. Keller; Gabriele Niedermann; Peter Van Endert

doi:10.1126/science.1172845

IRAP Identifies an Endosomal Compartment Required for MHC Class I Cross-Presentation

Loredana Saveanu(Délégation Paris 5), Oliver Carroll(Délégation Paris 5), Mirjana Weimershaus(Délégation Paris 5), Pierre Guermonprez(Inserm), Elke Firat(University Medical Center Freiburg), Viv Lindo(Wokingham Hospital), Fiona Greer(Wokingham Hospital), Jean Davoust(Délégation Paris 5), Roland Kratzer(Délégation Paris 5), Susanna R. Keller(University of Virginia), Gabriele Niedermann(University Medical Center Freiburg), Peter Van Endert(Délégation Paris 5)

Science

June 5, 2009

10.1126/science.1172845

Cited by 264

Abstract

Major histocompatibility complex (MHC) class I molecules present peptides, produced through cytosolic proteasomal degradation of cellular proteins, to cytotoxic T lymphocytes. In dendritic cells, the peptides can also be derived from internalized antigens through a process known as cross-presentation. The cellular compartments involved in cross-presentation remain poorly defined. We found a role for peptide trimming by insulin-regulated aminopeptidase (IRAP) in cross-presentation. In human dendritic cells, IRAP was localized to a Rab14+ endosomal storage compartment in which it interacted with MHC class I molecules. IRAP deficiency compromised cross-presentation in vitro and in vivo but did not affect endogenous presentation. We propose the existence of two pathways for proteasome-dependent cross-presentation in which final peptide trimming involves IRAP in endosomes and involves the related aminopeptidases in the endoplasmic reticulum.

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