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在小鼠淋巴瘤发生中,亚克隆突变选择鉴定出已知的癌症基因座,并提出新的候选基因。

Subclonal mutation selection in mouse lymphomagenesis identifies known cancer loci and suggests novel candidates.

机构信息

MRC London Institute of Medical Sciences (LMS), Du Cane Road, London, W12 0NN, UK.

Institute of Clinical Sciences (ICS), Faculty of Medicine, Imperial College London, Du Cane Road, London, W12 0NN, UK.

出版信息

Nat Commun. 2018 Jul 9;9(1):2649. doi: 10.1038/s41467-018-05069-9.

Abstract

Determining whether recurrent but rare cancer mutations are bona fide driver mutations remains a bottleneck in cancer research. Here we present the most comprehensive analysis of murine leukemia virus-driven lymphomagenesis produced to date, sequencing 700,000 mutations from >500 malignancies collected at time points throughout tumor development. This scale of data allows novel statistical approaches for identifying selected mutations and yields a high-resolution, genome-wide map of the selective forces surrounding cancer gene loci. We also demonstrate negative selection of mutations that may be deleterious to tumor development indicating novel avenues for therapy. Screening of two BCL2 transgenic models confirmed known drivers of human non-Hodgkin lymphoma, and implicates novel candidates including modifiers of immunosurveillance and MHC loci. Correlating mutations with genotypic and phenotypic features independently of local variance in mutation density also provides support for weakly evidenced cancer genes. An online resource http://mulv.lms.mrc.ac.uk allows customized queries of the entire dataset.

摘要

确定反复出现但罕见的癌症突变是否为真正的驱动突变仍然是癌症研究中的一个瓶颈。在这里,我们展示了迄今为止对鼠白血病病毒驱动的淋巴瘤发生进行的最全面分析,对整个肿瘤发展过程中收集的 500 多个恶性肿瘤中的超过 700,000 个突变进行了测序。这种规模的数据允许采用新的统计方法来识别选定的突变,并提供了围绕癌症基因座的选择压力的高分辨率全基因组图谱。我们还证明了对可能对肿瘤发展有害的突变的负选择,这表明了新的治疗途径。对两种 BCL2 转基因模型的筛选证实了已知的人类非霍奇金淋巴瘤的驱动因素,并暗示了包括免疫监视和 MHC 基因座调节剂在内的新候选因素。将突变与基因型和表型特征相关联,而不考虑突变密度的局部变化,也为弱证据的癌症基因提供了支持。一个在线资源 http://mulv.lms.mrc.ac.uk 允许对整个数据集进行定制查询。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c4b5/6037733/da11d6328bb1/41467_2018_5069_Fig1_HTML.jpg

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