Global proteogenomic analysis of human MHC class I-associated peptides derived from non-canonical reading frames

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作者
Céline M. Laumont
Tariq Daouda
Jean-Philippe Laverdure
Éric Bonneil
Olivier Caron-Lizotte
Marie-Pierre Hardy
Diana P. Granados
Chantal Durette
Sébastien Lemieux
Pierre Thibault
Claude Perreault
机构
[1] Institute for Research in Immunology and Cancer,Department of Medicine
[2] Université de Montréal,Department of Computer Science and Operations Research
[3] Faculty of Medicine,Department of Chemistry
[4] Université de Montréal,Division of Hematology
[5] Faculty of Arts and Sciences,undefined
[6] Université de Montréal,undefined
[7] Université de Montréal,undefined
[8] Hôpital Maisonneuve-Rosemont,undefined
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In view of recent reports documenting pervasive translation outside of canonical protein-coding sequences, we wished to determine the proportion of major histocompatibility complex (MHC) class I-associated peptides (MAPs) derived from non-canonical reading frames. Here we perform proteogenomic analyses of MAPs eluted from human B cells using high-throughput mass spectrometry to probe the six-frame translation of the B-cell transcriptome. We report that ∼10% of MAPs originate from allegedly noncoding genomic sequences or exonic out-of-frame translation. The biogenesis and properties of these ‘cryptic MAPs’ differ from those of conventional MAPs. Cryptic MAPs come from very short proteins with atypical C termini, and are coded by transcripts bearing long 3′UTRs enriched in destabilizing elements. Relative to conventional MAPs, cryptic MAPs display different MHC class I-binding preferences and harbour more genomic polymorphisms, some of which are immunogenic. Cryptic MAPs increase the complexity of the MAP repertoire and enhance the scope of CD8 T-cell immunosurveillance.
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