Department of Genome Sciences, University of Washington, Foege Building S-250, Box 355065, 1705 NE Pacific Street, Seattle, WA 98195-5065, USA.
Proc Natl Acad Sci U S A. 2009 Dec 22;106(51):21766-70. doi: 10.1073/pnas.0912499106. Epub 2009 Dec 7.
Recent large-scale cancer sequencing studies have focused primarily on identifying cancer-associated genes, but as an important byproduct provide "passenger mutation" data that can potentially illuminate the mutational mechanisms at work in cancer cells. Here, we explore patterns of nucleotide substitution in several cancer types using published data. We first show that selection (negative or positive) has affected only a small fraction of mutations, allowing us to attribute observed trends to underlying mutational processes rather than selection. We then show that the increased CpG mutation frequency observed in some cancers primarily occurs outside of CpG islands and CpG island shores, thus rejecting the hypothesis that the increase is a byproduct of island or shore methylation followed by deamination. We observe an A-->G vs. T-->C mutational asymmetry in some cancers similar to one that has been observed in germline mutations in transcribed regions, suggesting that the mutation process may be influenced by gene expression. We also demonstrate that the relative frequency of mutations at dinucleotide "hotspots" can be used as a tool to detect likely technical artifacts in large-scale studies.
最近的大规模癌症测序研究主要集中在鉴定与癌症相关的基因上,但作为一个重要的副产品,提供了“乘客突变”数据,这些数据有可能阐明癌细胞中的突变机制。在这里,我们使用已发表的数据来探索几种癌症类型中的核苷酸替换模式。我们首先表明,选择(负选择或正选择)只影响了一小部分突变,这使我们能够将观察到的趋势归因于潜在的突变过程,而不是选择。然后,我们表明,在一些癌症中观察到的 CpG 突变频率增加主要发生在 CpG 岛和 CpG 岛岸之外,从而否定了这种增加是岛或岸甲基化随后脱氨的副产物的假说。我们在一些癌症中观察到 A-->G 与 T-->C 的突变不对称性,类似于在转录区的种系突变中观察到的不对称性,这表明突变过程可能受到基因表达的影响。我们还证明,二核苷酸“热点”的突变相对频率可用作检测大规模研究中可能存在的技术伪影的工具。