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The C-terminal extension landscape of naturally presented HLA-I ligands.


ABSTRACT: HLA-I molecules play a central role in antigen presentation. They typically bind 9- to 12-mer peptides, and their canonical binding mode involves anchor residues at the second and last positions of their ligands. To investigate potential noncanonical binding modes, we collected in-depth and accurate HLA peptidomics datasets covering 54 HLA-I alleles and developed algorithms to analyze these data. Our results reveal frequent (442 unique peptides) and statistically significant C-terminal extensions for at least eight alleles, including the common HLA-A03:01, HLA-A31:01, and HLA-A68:01. High resolution crystal structure of HLA-A68:01 with such a ligand uncovers structural changes taking place to accommodate C-terminal extensions and helps unraveling sequence and structural properties predictive of the presence of these extensions. Scanning viral proteomes with the C-terminal extension motifs identifies many putative epitopes and we demonstrate direct recognition by human CD8+ T cells of a 10-mer epitope from cytomegalovirus predicted to follow the C-terminal extension binding mode.

SUBMITTER: Guillaume P 

PROVIDER: S-EPMC5960288 | biostudies-literature | 2018 May

REPOSITORIES: biostudies-literature

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The C-terminal extension landscape of naturally presented HLA-I ligands.

Guillaume Philippe P   Picaud Sarah S   Baumgaertner Petra P   Montandon Nicole N   Schmidt Julien J   Speiser Daniel E DE   Coukos George G   Bassani-Sternberg Michal M   Filippakopoulos Panagis P   Gfeller David D  

Proceedings of the National Academy of Sciences of the United States of America 20180430 20


HLA-I molecules play a central role in antigen presentation. They typically bind 9- to 12-mer peptides, and their canonical binding mode involves anchor residues at the second and last positions of their ligands. To investigate potential noncanonical binding modes, we collected in-depth and accurate HLA peptidomics datasets covering 54 HLA-I alleles and developed algorithms to analyze these data. Our results reveal frequent (442 unique peptides) and statistically significant C-terminal extension  ...[more]

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