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首页> 外文期刊>Human Molecular Genetics >Molecular evolution of multiple recurrent cancers of the bladder.
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Molecular evolution of multiple recurrent cancers of the bladder.

机译:多种复发性膀胱癌的分子进化。

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摘要

We describe the reconstruction of bladder tumor development in individual patients spanning periods of up to 17 years. Genomic alterations detected in the tumors were used for hierarchical cluster analysis of tumor subclones. The cluster analysis highlights the clonal relationship between tumors from each patient. Based on the cluster data we were able to reconstruct the evolution of tumors in a genetic tree, where tumors with few aberrations precede those with many genetic insults. The sequential order of the tumors in these pedigrees differs from the chronological order in which the tumors appear. Thus, a tumor with few alterations can be occult for years following removal of a more deranged derivative. Extensive genetic damage is seen to accumulate during the evolution of the tumors. To explain the type and extent of genetic damage in combination with the low stage and grade of these tumors, we hypothesize that in bladder cancer pathogenesis an increased rate of mitotic recombination is acquired early in the tumorigenic process.
机译:我们描述了个体患者长达17年的膀胱肿瘤发展的重建。在肿瘤中检测到的基因组改变被用于肿瘤亚克隆的分级聚类分析。聚类分析突出了每个患者肿瘤之间的克隆关系。基于聚类数据,我们能够在遗传树中重构肿瘤的进化,其中畸变少的肿瘤先于遗传损伤多的肿瘤。这些谱系中肿瘤的顺序与肿瘤出现的时间顺序不同。因此,去除更排列混乱的衍生物后,隐匿性很小的肿瘤可以隐匿多年。广泛的遗传损伤在肿瘤的发展过程中不断累积。为了解释遗传损伤的类型和程度,以及这些肿瘤的低分期和等级,我们假设在膀胱癌的发病机理中,在致瘤过程的早期就获得了有丝分裂重组率的提高。

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