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Peptide exchange on MHC-I by TAPBPR is driven by a negative allostery release cycle

Nat Chem Biol.. 2018-08; 
McShan AC, Natarajan K, Kumirov VK, Flores-Solis D, Jiang J, Badstübner M, Toor JS, Bagshaw CR, Kovrigin EL, Margulies DH, Sgourakis NG.
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Peptide Synthesis Unlabeled peptides (≥98% purity) were prepared by chemical synthesis (Biopeptek Inc., Malvern, PA, USA or GenScript, Piscataway, NJ, USA). Get A Quote

摘要

Chaperones TAPBPR and tapasin associate with class I major histocompatibility complexes (MHC-I) to promote optimization (editing) of peptide cargo. Here, we use solution NMR to investigate the mechanism of peptide exchange. We identify TAPBPR-induced conformational changes on conserved MHC-I molecular surfaces, consistent with our independently determined X-ray structure of the complex. Dynamics present in the empty MHC-I are stabilized by TAPBPR and become progressively dampened with increasing peptide occupancy. Incoming peptides are recognized according to the global stability of the final pMHC-I product and anneal in a native-like conformation to be edited by TAPBPR. Our results demonstrate an inverse relat... More

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