Literature DB >> 29331515

MHC class I loaded ligands from breast cancer cell lines: A potential HLA-I-typed antigen collection.

Dmitri V Rozanov1, Nikita D Rozanov2, Kami E Chiotti3, Ashok Reddy4, Phillip A Wilmarth4, Larry L David4, Seung W Cha5, Sunghee Woo6, Pavel Pevzner7, Vineet Bafna8, Gregory G Burrows9, Juha K Rantala10, Trevor Levin11, Pavana Anur3, Katie Johnson-Camacho3, Shaadi Tabatabaei3, Daniel J Munson12, Tullia C Bruno13, Jill E Slansky12, John W Kappler14, Naoto Hirano15, Sebastian Boegel16, Bernard A Fox17, Colt Egelston18, Diana L Simons18, Grecia Jimenez18, Peter P Lee18, Joe W Gray19, Paul T Spellman3.   

Abstract

To build a catalog of peptides presented by breast cancer cells, we undertook systematic MHC class I immunoprecipitation followed by elution of MHC class I-loaded peptides in breast cancer cells. We determined the sequence of 3196 MHC class I ligands representing 1921 proteins from a panel of 20 breast cancer cell lines. After removing duplicate peptides, i.e., the same peptide eluted from more than one cell line, the total number of unique peptides was 2740. Of the unique peptides eluted, more than 1750 had been previously identified, and of these, sixteen have been shown to be immunogenic. Importantly, half of these immunogenic peptides were shared between different breast cancer cell lines. MHC class I binding probability was used to plot the distribution of the eluted peptides in accordance with the binding score for each breast cancer cell line. We also determined that the tested breast cancer cells presented 89 mutation-containing peptides and peptides derived from aberrantly translated genes, 7 of which were shared between four or two different cell lines. Overall, the high throughput identification of MHC class I-loaded peptides is an effective strategy for systematic characterization of cancer peptides, and could be employed for design of multi-peptide anticancer vaccines. SIGNIFICANCE: By employing proteomic analyses of eluted peptides from breast cancer cells, the current study has built an initial HLA-I-typed antigen collection for breast cancer research. It was also determined that immunogenic epitopes can be identified using established cell lines and that shared immunogenic peptides can be found in different cancer types such as breast cancer and leukemia. Importantly, out of 3196 eluted peptides that included duplicate peptides in different cells 89 peptides either contained mutation in their sequence or were derived from aberrant translation suggesting that mutation-containing epitopes are on the order of 2-3% in breast cancer cells. Finally, our results suggest that interfering with MHC class I function is one of the mechanisms of how tumor cells escape immune system attack.
Copyright © 2018 The Authors. Published by Elsevier B.V. All rights reserved.

Entities:  

Keywords:  Breast cancer; MHC class I-restricted peptides; Neo-antigens; T cell-mediated immune response; Tumor associated antigens

Mesh:

Substances:

Year:  2018        PMID: 29331515      PMCID: PMC5999401          DOI: 10.1016/j.jprot.2018.01.004

Source DB:  PubMed          Journal:  J Proteomics        ISSN: 1874-3919            Impact factor:   4.044


  70 in total

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