Department of Chemistry, University of Virginia, Charlottesville, Virginia.
Department of Clinical Immunology, University of Birmingham, Birmingham, United Kingdom.
Cancer Immunol Res. 2017 May;5(5):376-384. doi: 10.1158/2326-6066.CIR-16-0280. Epub 2017 Mar 17.
Leukemias are highly immunogenic, but they have a low mutational load, providing few mutated peptide targets. Thus, the identification of alternative neoantigens is a pressing need. Here, we identify 36 MHC class I-associated peptide antigens with O-linked β--acetylglucosamine (-GlcNAc) modifications as candidate neoantigens, using three experimental approaches. Thirteen of these peptides were also detected with disaccharide units on the same residues and two contain either mono- and/or di-methylated arginine residues. A subset were linked with key cancer pathways, and these peptides were shared across all of the leukemia patient samples tested (5/5). Seven of the -GlcNAc peptides were synthesized and five (71%) were shown to be associated with multifunctional memory T-cell responses in healthy donors. An -GlcNAc-specific T-cell line specifically killed autologous cells pulsed with the modified peptide, but not the equivalent unmodified peptide. Therefore, these posttranslationally modified neoantigens provide logical targets for cancer immunotherapy. .
白血病具有高度的免疫原性,但突变负荷较低,提供的突变肽靶标较少。因此,鉴定替代的新抗原是当务之急。在这里,我们使用三种实验方法鉴定了 36 种 MHC Ⅰ类相关的带有 O 连接的β--乙酰氨基葡萄糖(-GlcNAc)修饰的肽抗原作为候选新抗原。其中 13 种肽在相同的残基上也检测到二糖单位,两种含有单甲基和/或二甲基精氨酸残基。其中一部分与关键的癌症途径有关,这些肽在所有测试的白血病患者样本中都有共享(5/5)。七种 -GlcNAc 肽被合成,其中五种(71%)在健康供体中显示与多功能记忆 T 细胞反应有关。一种 -GlcNAc 特异性 T 细胞系特异性地杀死用修饰肽脉冲的自身细胞,但不能杀死等效的未修饰肽。因此,这些翻译后修饰的新抗原为癌症免疫治疗提供了合理的靶标。
