4.8 Article

MHC class I-associated peptides derive from selective regions of the human genome

Journal

JOURNAL OF CLINICAL INVESTIGATION
Volume 126, Issue 12, Pages 4690-4701

Publisher

AMER SOC CLINICAL INVESTIGATION INC
DOI: 10.1172/JCI88590

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Funding

  1. Quebec Breast Cancer Foundation
  2. Genome Canada Innovation Network
  3. CIBC Breast Cancer Research Chair at Universite de Montreal
  4. Katelyn Bedard Bone Marrow Association

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MHC class I-associated peptides (MAPs) define the immune self for CD8(+) T lymphocytes and are key targets of cancer immunosurveillance. Here, the goals of our work were to determine whether the entire set of protein-coding genes could generate MAPs and whether specific features influence the ability of discrete genes to generate MAPs. Using proteogenomics, we have identified 25,270 MAPs isolated from the B lymphocytes of 18 individuals who collectively expressed 27 highfrequency HLA-A, B allotypes. The entire MAP repertoire presented by these 27 allotypes covered only 10% of the exomic sequences expressed in B lymphocytes. Indeed, 41% of expressed protein-coding genes generated no MAPs, while 59% of genes generated up to 64 MAPs, often derived from adjacent regions and presented by different allotypes. We next identified several features of transcripts and proteins associated with efficient MAP production. From these data, we built a logistic regression model that predicts with good accuracy whether a gene generates MAPs. Our results show preferential selection of MAPs from a limited repertoire of proteins with distinctive features. The notion that the MHC class I immunopeptidome presents only a small fraction of the protein-coding genome for monitoring by the immune system has profound implications in autoimmunity and cancer immunology.

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