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Spatial Intratumor Genomic Heterogeneity within Localized Prostate Cancer Revealed by Single-nucleus Sequencing

机译:单核测序揭示局部前列腺癌内的空间肿瘤内基因组异质性

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摘要

BackgroundProstate adenocarcinoma (PCa) is a complex genetic disease, and the implementation of personalized treatment in PCa faces challenges due to significant inter- and intrapatient tumor heterogeneities. ObjectiveTo systematically explore the genomic complexity of tumor cells with different Gleason scores (GSs) in PCa. Design, setting, and participantsWe performed single-cell whole genome sequencing of 17 tumor cells from localized lesions with distinct GS and matched four normal samples from two prostatectomy patients. Outcome measurements and statistical analysisAll classes of genomic alterations were identified, including substitutions, insertions/deletions, copy number alterations, and rearrangements. Results and limitationsSignificant spatial, intra- and intertumoral heterogeneities were observed at the cellular level. In the patient 1, all cells shared the sameTP53driver mutation, implying a monoclonal origin of PCa. In the patient 2, only a subpopulation of cells contained theTP53driver mutation, whereas other cells carried different driver mutations, indicating a typical polyclonal model with separate clonal cell expansions. The tumor cells from different sides of prostate owned various mutation patterns. Considerable neoantigens were predicted among different cells, implying unknown immune editing components helping prostate tumor cells escaping from immune surveillance. ConclusionsThere is a significant spatial genomic heterogeneity even in the same PCa patient. Our study also provides the first genome-wide evidence at single-cell level, supporting that the origin of PCa could be either polyclonal or monoclonal, which has implications for treatment decisions for prostate cancer. Patient summaryWe reported the first single-cell whole genomic data of prostate adenocarcinoma (PCa) from different Gleason scores. Identification of these genetic alterations may help understand PCa tumor progression and clonal evolution.
机译:背景抗原腺癌(PCA)是一种复杂的遗传疾病,并且由于显着和内裤内肿瘤异质性,PCA中个性化治疗的实施面临挑战。 ObjectiveTo系统地探讨了PCA中具有不同GLOASON细胞的肿瘤细胞基因组复杂性。设计,设定和参与者在具有不同GS的局部病变中进行了17个肿瘤细胞的单细胞全基因组测序,并匹配来自两个前列腺切除术患者的四个正常样本。结果测量和统计分析统计分析阶类基因组改变,包括替代,插入/缺失,拷贝数改变和重排。在细胞水平下观察结果和限制性义症,在细胞水平下观察到的间间异质性。在患者1中,所有细胞共用SametP53Driver突变,暗示PCA的单克隆源。在患者2中,仅含有ThetP53Driver突变的细胞亚群,而其他细胞携带不同的驾驶员突变,表明具有单独的克隆细胞膨胀的典型多克隆模型。来自前列腺不同侧面的肿瘤细胞拥有各种突变模式。在不同的细胞之间预测了相当大的新稻草原,暗示了有效的免疫编辑组分,帮助前列腺肿瘤细胞从免疫监测中逸出。结论即使在同一PCA患者中也是一个重要的空间基因组异质性。我们的研究还提供了在单细胞层面的第一种基因组据提供,支持PCA的起源可以是多克隆或单克隆,这对前列腺癌进行治疗决策具有影响。患者摘要我们报道了来自不同GLEAN分数的前列腺腺癌(PCA)的第一个单细胞全基因组数据。鉴定这些遗传改变可能有助于了解PCA肿瘤进展和克隆演化。

著录项

  • 来源
    《European urology》 |2018年第5期|共9页
  • 作者单位

    Department of Pathology Beijing Hospital National Center of Gerontology;

    Department of Pathology Beijing Hospital National Center of Gerontology;

    Department of Urology Beijing Hospital National Center of Gerontology;

    Department of Urology Beijing Hospital National Center of Gerontology;

    Department of Urology Beijing Hospital National Center of Gerontology;

    Department of Oncology Beijing Hospital National Center of Gerontology;

    Department of Urology Beijing Hospital National Center of Gerontology;

    Department of Urology Beijing Hospital National Center of Gerontology;

    Department of Pathology Beijing Hospital National Center of Gerontology;

    Department of Pathology Beijing Hospital National Center of Gerontology;

    The Key Laboratory of Geriatrics Beijing Hospital National Center of Gerontology;

    The Key Laboratory of Geriatrics Beijing Hospital National Center of Gerontology;

    The Key Laboratory of Geriatrics Beijing Hospital National Center of Gerontology;

    Department of Oncology Beijing Hospital National Center of Gerontology;

    Sun Yat-sen University Cancer Center;

    Center for Biotherapy Beijing Hospital National Center of Gerontology;

    Department of Pathology Beijing Hospital National Center of Gerontology;

    Department of Urology Beijing Hospital National Center of Gerontology;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 泌尿科学(泌尿生殖系疾病);
  • 关键词

    Gleason score; Neoantigen; Prostate cancer; Single-nucleus sequencing; Tumor heterogeneity;

    机译:Gleason得分;新南古;前列腺癌;单核测序;肿瘤异质性;

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