Exploration of peptides bound to MHC class I molecules in melanoma |
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| Authors: | Antonia L. Pritchard Marcus L. Hastie Michelle Neller Jeffrey J. Gorman Chris W. Schmidt Nicholas K. Hayward |
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| Affiliation: | 1. Oncogenomics Research Group, QIMR Berghofer Medical Research Institute, Herston, Brisbane, Qld, Australia;2. Protein Discovery Centre, QIMR Berghofer Medical Research Institute, Herston, Brisbane, Qld, Australia;3. Cancer Immunotherapy Group, QIMR Berghofer Medical Research Institute, Herston, Brisbane, Qld, Australia |
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| Abstract: | Advancements in high‐resolution HPLC and mass spectrometry have reinvigorated the application of this technology to identify peptides eluted from immunopurified MHC class I molecules. Three melanoma cell lines were assessed using w6/32 isolation, peptide elution and HPLC purification; peptides were identified by mass spectrometry. A total of 13 829 peptides were identified; 83–87% of these were 8–11 mers. Only approximately 15% have been described before. Subcellular locations of the source proteins showed even sampling; mRNA expression and total protein length were predictive of the number of peptides detected from a single protein. HLA‐type binding prediction for 10 078 9/10 mer peptides assigned 88–95% to a patient‐specific HLA subtype, revealing a disparity in strength of predicted binding. HLA‐B*27‐specific isolation successfully identified some peptides not found using w6/32. Sixty peptides were selected for immune screening, based on source protein and predicted HLA binding; no new peptides recognized by antimelanoma T cells were discovered. Additionally, mass spectrometry was unable to identify several epitopes targeted ex vivo by one patient's T cells. |
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| Keywords: | melanoma mass spectrometry MHC class I proteome antigen epitope peptide |
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