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首页> 外文期刊>Human Molecular Genetics >Inferring primary tumor sites from mutation spectra: A meta-analysis of histology-specific aberrations in cancer-derived cell lines
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Inferring primary tumor sites from mutation spectra: A meta-analysis of histology-specific aberrations in cancer-derived cell lines

机译:从突变谱图推断原发性肿瘤位点:荟萃分析组织学特异畸变在癌症衍生细胞系中

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摘要

Next-generation sequencing technologies have led to profound characterization of mutation spectra for several cancer types. Hence, we sought to systematically compare genomic aberrations between primary tumors and cancer lines. For this, we compiled publically available sequencing data of 1651 genes across 905 cell lines. We used them to characterize 23 distinct primary tumor sites by a novel approach that is based on Bayesian spam-filtering techniques. Thereby, we confirmed the strong overall similarity of alterations between patient samples and cell culture. However, we also identified several suspicious mutations, which had not been associated with their cancer types before. Based on these characterizations, we developed the inferring cancer origins from mutation spectra (ICOMS) tool. On our cell line collection, the algorithm reached a prediction specificity rate of 79%, which strongly variegated between primary cancer sites. On an independent validation cohort of 431 primary tumor samples, we observed a similar accuracy of 71%. Additionally, we found that ICOMS could be employed to deduce further attributes from mutation spectra, including sub-histology and compound sensitivity. Thus, thorough classification of site-specific mutation spectra for cell lines may decipher further genome-phenotype associations in cancer.
机译:下一代测序技术已导致对几种癌症类型的突变谱进行深刻表征。因此,我们试图系统地比较原发性肿瘤和癌症细胞系之间的基因组畸变。为此,我们汇总了905个细胞系中1651个基因的公开测序数据。我们使用它们基于贝叶斯垃圾邮件过滤技术的新颖方法来表征23个不同的原发肿瘤部位。因此,我们证实了患者样品和细胞培养物之间变化的总体相似性。但是,我们还发现了一些可疑的突变,这些突变以前与它们的癌症类型无关。基于这些特征,我们开发了根据突变谱(ICOMS)工具推断癌症起源的方法。在我们的细胞系收集中,该算法的预测特异性率为79%,在原发癌部位之间存在很大差异。在431个原发性肿瘤样本的独立验证队列中,我们观察到了71%的相似准确性。此外,我们发现ICOMS可用于从突变谱中推断出更多属性,包括亚组织学和化合物敏感性。因此,对细胞系的位点特异性突变谱进行彻底分类可能会破译癌症中进一步的基因组-表型关联。

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