Publication | Open Access
Recycling MHC class I molecules and endosomal peptide loading
296
Citations
26
References
1999
Year
Class Ii MoleculesPresent PeptidesMhc ClassProtein FoldingPeptide LibraryHla ImmunogeneticsImmunologyCell TraffickingMolecular BiologyVirologyAntigen ProcessingCytoskeletonProtein TransportIntracellular TraffickingViral Structural ProteinEndosomal Peptide LoadingMedicineCell Biology
MHC class I molecules usually present peptides derived from endogenous antigens that are bound in the endoplasmic reticulum. Loading of exogenous antigens on class I molecules, e.g., in cross-priming, sometimes occurs, but the intracellular location where interaction between the antigenic fragment and class I takes place is unclear. Here we show that measles virus F protein can be presented by class I in transporters associated with antigen processing-independent, NH(4)Cl-sensitive manner, suggesting that class I molecules are able to interact and bind antigen in acidic compartments, like class II molecules. Studies on intracellular transport of green fluorescent protein-tagged class I molecules in living cells confirmed that a small fraction of class I molecules indeed enters classical MHC class II compartments (MIICs) and is transported in MIICs back to the plasma membrane. Fractionation studies show that class I complexes in MIICs contain peptides. The pH in MIIC (around 5.0) is such that efficient peptide exchange can occur. We thus present evidence for a pathway for class I loading that is shared with class II molecules.
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