MHC-II dynamics are maintained in HLA-DR allotypes to ensure catalyzed peptide exchange

Author:

Abualrous Esam T.ORCID,Stolzenberg Sebastian,Sticht JanaORCID,Wieczorek Marek,Roske Yvette,Günther Matthias,Dähn Steffen,Boesen Benedikt B.,Calvo Marcos MartínezORCID,Biese Charlotte,Kuppler Frank,Medina-García Álvaro,Álvaro-Benito MiguelORCID,Höfer ThomasORCID,Noé FrankORCID,Freund ChristianORCID

Abstract

AbstractPresentation of antigenic peptides by major histocompatibility complex class II (MHC-II) proteins determines T helper cell reactivity. The MHC-II genetic locus displays a large degree of allelic polymorphism influencing the peptide repertoire presented by the resulting MHC-II protein allotypes. During antigen processing, the human leukocyte antigen (HLA) molecule HLA-DM (DM) encounters these distinct allotypes and catalyzes exchange of the placeholder peptide CLIP by exploiting dynamic features of MHC-II. Here, we investigate 12 highly abundant CLIP-bound HLA-DRB1 allotypes and correlate dynamics to catalysis by DM. Despite large differences in thermodynamic stability, peptide exchange rates fall into a target range that maintains DM responsiveness. A DM-susceptible conformation is conserved in MHC-II molecules, and allosteric coupling between polymorphic sites affects dynamic states that influence DM catalysis. As exemplified for rheumatoid arthritis, we postulate that intrinsic dynamic features of peptide–MHC-II complexes contribute to the association of individual MHC-II allotypes with autoimmune disease.

Publisher

Springer Science and Business Media LLC

Subject

Cell Biology,Molecular Biology

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