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Literature DB >> 25605945

The first step of peptide selection in antigen presentation by MHC class I molecules.

Malgorzata A Garstka¹, Alexander Fish², Patrick H N Celie², Robbie P Joosten², George M C Janssen³, Ilana Berlin¹, Rieuwert Hoppes¹, Magda Stadnik², Lennert Janssen¹, Huib Ovaa¹, Peter A van Veelen³, Anastassis Perrakis², Jacques Neefjes⁴.

Abstract

MHC class I molecules present a variable but limited repertoire of antigenic peptides for T-cell recognition. Understanding how peptide selection is achieved requires mechanistic insights into the interactions between the MHC I and candidate peptides. We find that, at first encounter, MHC I H-2K(b) considers a wide range of peptides, including those with expanded N termini and unfitting anchor residues. Discrimination occurs in the second step, when noncanonical peptides dissociate with faster exchange rates. This second step exhibits remarkable temperature sensitivity, as illustrated by numerous noncanonical peptides presented by H-2K(b) in cells cultured at 26 °C relative to 37 °C. Crystallographic analyses of H-2K(b)-peptide complexes suggest that a conformational adaptation of H-2K(b) drives the decisive step in peptide selection. We propose that MHC class I molecules consider initially a large peptide pool, subsequently refined by a temperature-sensitive induced-fit mechanism to retain the canonical peptide repertoire.

Keywords: anchor residues; antigen presentation; dynamics; entropy; peptide binding

Mesh：

Substances：

Year: 2015 PMID： 25605945 PMCID： PMC4321303 DOI： 10.1073/pnas.1416543112

Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN： 0027-8424 Impact factor: 11.205

35 in total

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