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TAPBPR employs a ligand-independent docking mechanism to chaperone MR1 molecules

Nat Chem Biol. 2022-06; 
Andrew C McShan, Christine A Devlin, Georgia F Papadaki, Yi Sun, Adam I Green, Giora I Morozov, George M Burslem, Erik Procko, Nikolaos G Sgourakis
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Catalog Peptides … MHC-I peptides used for refolding were prepared by chemical synthesis (Biopeptek Inc. or GenScript): photoA02 (KILGFVFJV, where J is the photolabile 3-amino-3-(2-nitrophenyl)-… Get A Quote

摘要

Chaperones tapasin and transporter associated with antigen processing (TAP)-binding protein related (TAPBPR) associate with the major histocompatibility complex (MHC)-related protein 1 (MR1) to promote trafficking and cell surface expression. However, the binding mechanism and ligand dependency of MR1/chaperone interactions remain incompletely characterized. Here in vitro, biochemical and computational studies reveal that, unlike MHC-I, TAPBPR recognizes MR1 in a ligand-independent manner owing to the absence of major structural changes in the MR1 α helix between empty and ligand-loaded molecules. Structural characterization using paramagnetic nuclear magnetic resonance experiments combined with restrained mol... More

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