Title : Insights into MHC class I peptide loading from the structure of the
tapasin-
ERp57 thiol oxidoreductase
heterodimer
Abstract :
- Tapasin is a glycoprotein critical for loading major histocompatibility complex (MHC) class I molecules with high-affinity peptides
- It functions within the multimeric peptide-loading complex ( PLC ) as a disulfide-linked, stable heterodimer with the thiol oxidoreductase ERp57 , and this covalent interaction is required to support optimal PLC activity
- Here, we present the 2.6 A resolution structure of the tapasin- ERp57 core of the PLC
- The structure revealed that tapasin interacts with both ERp57 catalytic domains , accounting for the stabil ity of th e hetero dimer, and provided an example of a protein disulfide isomerase family member interacting with substrate
- Mutational analysis identified a conserved surface on tapasin that interacted with MHC class I molecules and was critical for peptide loading and editing functions of the tapasin- ERp57 heterodimer
- By combining the tapasin- ERp57 structure with those of other defined PLC components, we present a molecular model that illuminates the processes involved in MHC class I peptide loading
Output (sent_index, trigger,
protein,
sugar,
site):
- 1. glycoprotein, , Tapasin, -, -
- 1. glycoprotein, , glycoprotein, -, -
Output(Part-Of) (sent_index,
protein,
site):
*Output_Site_Fusion* (sent_index,
protein,
sugar,
site):