4.6 Article

Breast Cancer Neoantigens Can Induce CD8+ T-Cell Responses and Antitumor Immunity

Journal

CANCER IMMUNOLOGY RESEARCH
Volume 5, Issue 7, Pages 516-523

Publisher

AMER ASSOC CANCER RESEARCH
DOI: 10.1158/2326-6066.CIR-16-0264

Keywords

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Funding

  1. Susan G. Komen for the Cure [KG111025]
  2. Siteman Cancer Center/Barnes-Jewish Hospital Foundation Cancer Frontier Fund [BJHF CFF 7538-55]
  3. Siteman Cancer Center Siteman Investment Program [SIPPre-SPORE 3781]
  4. NCI [T32 CA 009621]
  5. NIH [P30CA091842]

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Next-generation sequencing technologies have provided insights into the biology and mutational landscape of cancer. Here, we evaluate the relevance of cancer neoantigens in human breast cancers. Using patient-derived xenografts from three patients with advanced breast cancer (xenografts were designated as WHIM30, WHIM35, and WHIM37), we sequenced exomes of tumor and patient- matched normal cells. We identified 2,091 (WHIM30), 354 (WHIM35), and 235 (WHIM37) nonsynonymous somatic mutations. A computational analysis identified and prioritized HLA class I-restricted candidate neoantigens expressed in the dominant tumor clone. Each candidate neoantigen was evaluated using peptide-binding assays, T-cell cultures that measure the ability of CD8(+) T cells to recognize candidate neoantigens, and preclinical models in which we measured antitumor immunity. Our results demonstrate that breast cancer neoantigens can be recognized by the immune system, and that human CD8(+) T cells enriched for prioritized breast cancer neoantigens were able to protect mice from tumor challenge with autologous patient- derived xenografts. We conclude that next-generation sequencing and epitope-prediction strategies can identify and prioritize candidate neoantigens for immune targeting in breast cancer. (C)2017 AACR.

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