Unlike
other glycoproteins, correct folding of MHC class I molecules is not
sufficient to trigger their exit from the ER, they exit only after
peptide loading.
Described here is the process of antigen presentation
which consists of the folding, assembly, and peptide loading of MHC
class I molecules.
The newly synthesized MHC class I Heavy Chain (HC) is
initially folded with the help of several chaperones (calnexin, BiP,
ERp57) and then binds with Beta-2-microglobulin (B2M).
This MHC:B2M
heterodimer enters the peptide loading complex (PLC), a multiprotein
complex that includes calreticulin, endoplasmic reticulum resident
protein 57 (ERp57), transporter associated with antigen processing (TAP)
and tapasin.
Peptides generated from Ub-proteolysis are transported
into the ER through TAP. These peptides are further trimmed by
ER-associated aminopeptidase (ERAP) and loaded on to MHC class I
molecules. Stable MHC class I trimers with high-affinity peptide are
transported from the ER to the cell surface by the Golgi apparatus.
- from REACTOME source record: REACT_75795
- Taxonomic scope :
- organism-specific biosystem
- Organism :
- Homo sapiens
- BSID:
- 366163
Type: pathway
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