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首页> 外文期刊>Molecular medicine reports >Identification of recurrent and novel mutations by whole-genome sequencing of colorectal tumors from the Han population in Shanghai, eastern China
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Identification of recurrent and novel mutations by whole-genome sequencing of colorectal tumors from the Han population in Shanghai, eastern China

机译:中国东部上海汉族人群结直肠肿瘤全基因组序列鉴定

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摘要

Previous studies have identified recurrent oncogenic mutations in colorectal cancer (CRC), but there is limited CRC genomic data from the Chinese Han population. Whole-genome sequencing was performed on 10 primary CRC tumors and matched adjacent normal tissues from patients from the Han population in Shanghai, at an average of 27.8x and 27.9x coverage, respectively. In the 10 tumor samples, 32 significant somatic mutated genes were identified, 13 of which were also reported as CRC mutations in The Cancer Genome Atlas Network. All the mutated genes were enriched in functions associated with channel activity, which has rarely been reported in previous studies investigating CRC. Furthermore, 21 chromosomal rearrangements were detected and 4 rearrangements encoded predicted in-frame fusion proteins, including a fusion of phosphorylase kinase regulatory subunit b and NOTCH2 demonstrated in 2 out of 10 tumors. Chromosome 8 was amplified in 1 tumor and chromosome 20 was amplified in 2 out of 10 CRC patients. The present study produced a genomic mutation profile of CRC, which provides a valuable resource for further insight into the mutations that characterize CRC in patients from the Han population in Shanghai, eastern China.
机译:以前的研究已经确定了结直肠癌(CRC)中的复发性致癌突变,但来自中国汉族人群的CRC基因组数据有限。在10个主要CRC肿瘤上进行全基因组测序,并分别与上海汉族人群的患者相匹配,平均分别为27.8倍和27.9x覆盖率。在10个肿瘤样品中,鉴定了32种显着的体细胞突变基因,其中13种也被报告为癌症基因组Atlas网络中的CRC突变。所有突变的基因富集在与信道活动相关的功能中,这很少在先前研究CRC的研究中报道。此外,检测到21个染色体重排,并且4个重排编码预测的内框内融合蛋白,包括磷酸化酶激酶调节亚基B和Notch2的融合,其中10个肿瘤中的2个。在10名CRC患者中,在1颗肿瘤中扩增染色体8,染色体20分别为2分。本研究制作了CRC的基因组突变谱,其提供了一种有价值的资源,用于进一步了解从中国东部地上上海汉族人口患者表征CRC的突变。

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  • 来源
    《Molecular medicine reports》 |2018年第2期|共10页
  • 作者

    Teng Hongfei; Gao Renyuan; Qin Nan; Jiang Xun; Ren Min; Wang Yu; Wu Shouxin; Li Ning; Zhao Jiangman; Qin Huanlong;

  • 作者单位

    Tongji Univ Sch Med Shanghai Peoples Hosp 10 Dept Gen Surg 301 Middle Yanchang Rd Shanghai;

    Tongji Univ Sch Med Shanghai Peoples Hosp 10 Dept Gen Surg 301 Middle Yanchang Rd Shanghai;

    Tongji Univ Sch Med Shanghai Peoples Hosp 10 Dept Gut Microbiota Diag &

    Treatment Shanghai;

    Tongji Univ Sch Med Shanghai Peoples Hosp 10 Dept Gen Surg 301 Middle Yanchang Rd Shanghai;

    Biotecan Med Diagnost Co Ltd Dept Med Zhangjiang Ctr Translat Med 180 Zhangheng Rd Shanghai;

    Biotecan Med Diagnost Co Ltd Dept Med Zhangjiang Ctr Translat Med 180 Zhangheng Rd Shanghai;

    Biotecan Med Diagnost Co Ltd Dept Med Zhangjiang Ctr Translat Med 180 Zhangheng Rd Shanghai;

    Tongji Univ Sch Med Shanghai Peoples Hosp 10 Dept Gut Microbiota Diag &

    Treatment Shanghai;

    Biotecan Med Diagnost Co Ltd Dept Med Zhangjiang Ctr Translat Med 180 Zhangheng Rd Shanghai;

    Tongji Univ Sch Med Shanghai Peoples Hosp 10 Dept Gen Surg 301 Middle Yanchang Rd Shanghai;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 基础医学;
  • 关键词

    colorectal cancer; whole-genome sequencing; chromosomal rearrangement; copy number variation;

    机译:结直肠癌;全基因组测序;染色体重排;拷贝数变异;

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