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首页> 外文期刊>Cancer immunology research. >Exome Sequencing to Predict Neoantigens in Melanoma
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Exome Sequencing to Predict Neoantigens in Melanoma

机译:外显子组测序可预测黑色素瘤中的新抗原

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The ability to use circulating peripheral blood cells and matched tumor sequencing data as a basis for neoantigen prediction has exciting possibilities for application in the personalized treatment of cancer patients. Wehave used a high-throughput screening approach, combining whole-exome sequence data, mRNA microarrays, and publicly available epitope prediction algorithm output to identify mutated proteins processed and displayed by patient tumors and recognized by circulating immune cells. Matched autologous melanoma cell lines and peripheral blood mononuclear cells were used to create mixed lymphocyte tumor cell cultures, resulting in an expansion of tumor-reactive T cells to use for mutated peptide screening. Five patients were investigated, three of whom had a durable complete response (CR; 15+ years) in an autologous melanoma-pulsed dendritic cell clinical trial. We identified seven mutated antigens in total that stimulated T-effector memory cells in two of the five patients. While the procedure did not result in clinically applicable neoantigens for all patients, those identified were likely important in tumor clearance, leading to durable CR. The nature of the screening process allows results to be obtained rapidly and is easily applicable to a wide variety of different tumor types. (C) 2015 AACR.
机译:使用循环外周血细胞和匹配的肿瘤测序数据作为新抗原预测基础的能力为在癌症患者的个性化治疗中应用提供了令人兴奋的可能性。我们使用了高通量筛选方法,结合了全外显子序列数据,mRNA微阵列和公开可用的表位预测算法输出,以识别由患者肿瘤加工和展示并被循环免疫细胞识别的突变蛋白。匹配的自体黑素瘤细胞系和外周血单核细胞被用于创建混合的淋巴细胞肿瘤细胞培养物,从而导致肿瘤反应性T细胞扩增,用于突变肽筛选。在一项自体黑色素瘤脉冲树突状细胞临床试验中,对五名患者进行了研究,其中三名具有持久的完全缓解(CR; 15年以上)。我们鉴定出总共刺激了五名患者中的两名的T效应记忆细胞的七个突变抗原。尽管该程序并未在所有患者中产生临床适用的新抗原,但已鉴定出的新抗原可能对清除肿瘤很重要,从而导致持久的CR。筛选过程的性质使得可以快速获得结果,并容易适用于多种不同的肿瘤类型。 (C)2015 AACR。

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