Summary MHC-I Genotype Restricts the Oncogenic Mutational Landscape
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MHC-I Genotype Restricts the Oncogenic Mutational Landscape

机译:MHC-I基因型限制了致癌突变

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SummaryMHC-I molecules expose the intracellular protein content on the cell surface, allowing T?cells to detect foreign or mutated peptides. The combination of six MHC-I alleles each individual carries defines the sub-peptidome that can be effectively presented. We applied this concept to human cancer, hypothesizing that oncogenic mutations could arise in gaps in personal MHC-I presentation. To validate this hypothesis, we developed and applied a residue-centric patient presentation score to 9,176 cancer patients across 1,018 recurrent oncogenic mutations. We found that patient MHC-I genotype-based scores could predict which mutations were more likely to emerge in their tumor. Accordingly, poor presentation of a mutation across patients was correlated with higher frequency among tumors. These results support that MHC-I genotype-restricted immunoediting during tumor formation shapes the landscape of oncogenic mutations observed in clinically diagnosed tumors and paves the way for predicting personal cancer susceptibilities from knowledge of MHC-I genotype.Graphical AbstractDisplay OmittedHighlights
机译:<![cdata [ 摘要 MHC-I分子暴露细胞表面上的细胞内蛋白质含量,允许T 2细胞检测异物或突变的肽。六种MHC-I等位基因的组合每个单独的携带定义可以有效地呈现的副肽。我们将这种概念应用于人类癌症,假设致癌突变可能在个人MHC-i呈现中出现差距。为了验证这一假设,我们开发并将残留物患者呈现得分达到9,176名癌症患者,横跨1,018个复发性致癌突变。我们发现患者MHC-I基因型的评分可以预测其在肿瘤中更容易出现的突变。因此,对患者的突变的差异不良与肿瘤中较高的频率相关。这些结果支持MHC-I基因型限制在肿瘤形成期间的免疫性造型在临床诊断的肿瘤中观察到的致癌突变景观,并从MHC-I基因型知识中铺平了预测个人癌症敏感性的方式。 图形抽象 显示省略 亮点

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