Department of Surgery, Washington University School of Medicine, St. Louis, Missouri.
McDonnell Genome Institute, Washington University School of Medicine, St. Louis, Missouri.
Cancer Immunol Res. 2017 Jul;5(7):516-523. doi: 10.1158/2326-6066.CIR-16-0264. Epub 2017 Jun 15.
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. .
下一代测序技术为癌症的生物学和突变景观提供了深入的了解。在这里,我们评估了人类乳腺癌中癌症新抗原的相关性。使用来自三名晚期乳腺癌患者的患者来源异种移植物(异种移植物被指定为 WHIM30、WHIM35 和 WHIM37),我们对肿瘤和患者匹配的正常细胞进行了外显子组测序。我们鉴定了 2091 个(WHIM30)、354 个(WHIM35)和 235 个(WHIM37)非同义体细胞突变。计算分析确定并优先考虑了在优势肿瘤克隆中表达的 HLA 类 I 受限的候选新抗原。使用肽结合测定、测量 CD8 T 细胞识别候选新抗原能力的 T 细胞培养物以及我们测量抗肿瘤免疫的临床前模型来评估每个候选新抗原。我们的结果表明,乳腺癌新抗原可以被免疫系统识别,并且富含优先考虑的乳腺癌新抗原的人类 CD8 T 细胞能够保护小鼠免受同源患者来源异种移植物的肿瘤挑战。我们得出结论,下一代测序和表位预测策略可以识别和优先考虑针对乳腺癌免疫靶向的候选新抗原。
