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Immunology

Epitope Landscape in Breast and Colorectal Cancer

Neil H. Segal, D. Williams Parsons, Karl S. Peggs, Victor Velculescu, Ken W. Kinzler, Bert Vogelstein and James P. Allison
Neil H. Segal
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D. Williams Parsons
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Karl S. Peggs
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Victor Velculescu
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Ken W. Kinzler
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Bert Vogelstein
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James P. Allison
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DOI: 10.1158/0008-5472.CAN-07-3095 Published February 2008
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Abstract

The finding that individual cancers contain many mutant genes not present in normal tissues has prompted considerable interest in the cancer epitope landscape. To further understand such effects, we applied in silico–based epitope prediction algorithms and high throughput post hoc analysis to identify candidate tumor antigens. Analysis of 1,152 peptides containing missense mutations previously identified in breast and colorectal cancer revealed that individual cancers accumulate on average ∼10 and ∼7 novel and unique HLA-A*0201 epitopes, respectively, including genes implicated in the neoplastic process. These data suggest that, with appropriate manipulation of the immune system, tumor cell destruction in situ may provide a polyvalent tumor vaccine without a requirement for knowledge of the targeted antigens. [Cancer Res 2008;68(3):889–92]

  • genomic instability
  • tumor antigens
  • HLA

Footnotes

    • Received August 13, 2007.
    • Revision received October 24, 2007.
    • Accepted November 20, 2007.
    • ©2008 American Association for Cancer Research.
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    Cancer Research: 68 (3)
    February 2008
    Volume 68, Issue 3
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    Epitope Landscape in Breast and Colorectal Cancer
    Neil H. Segal, D. Williams Parsons, Karl S. Peggs, Victor Velculescu, Ken W. Kinzler, Bert Vogelstein and James P. Allison
    Cancer Res February 1 2008 (68) (3) 889-892; DOI: 10.1158/0008-5472.CAN-07-3095

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    Epitope Landscape in Breast and Colorectal Cancer
    Neil H. Segal, D. Williams Parsons, Karl S. Peggs, Victor Velculescu, Ken W. Kinzler, Bert Vogelstein and James P. Allison
    Cancer Res February 1 2008 (68) (3) 889-892; DOI: 10.1158/0008-5472.CAN-07-3095
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