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在一个 AML 病例中进行了长达 9 年的克隆动力学研究,揭示了白血病进展的复杂性。

Clonal dynamics in a single AML case tracked for 9 years reveals the complexity of leukemia progression.

机构信息

Department of Computer Science, University of Toronto, Toronto, Ontario, Canada.

The Donnelly Centre for Cellular and Biomolecular Research, University of Toronto, Toronto, Ontario, Canada.

出版信息

Leukemia. 2016 Feb;30(2):295-302. doi: 10.1038/leu.2015.264. Epub 2015 Oct 1.

Abstract

Most types of cancers are made up of heterogeneous mixtures of genetically distinct subclones. In particular, acute myeloid leukemia (AML) has been shown to undergo substantial clonal evolution over the course of the disease. AML tends to harbor fewer mutations than solid tumors, making it challenging to infer clonal structure. Here, we present a 9-year, whole-exome sequencing study of a single case at 12 time points, from the initial diagnosis until a fourth relapse, including 6 remission samples in between. To the best of our knowledge, it covers the longest time span of any data set of its kind. We used these time series data to track the hierarchy and order of variant acquisition, and subsequently analyzed the evolution of somatic variants to infer clonal structure. From this, we postulate the development and extinction of subclones, as well as their anticorrelated expansion via varying drug responses. In particular, we show that new subclones started appearing after the first complete remission. The presence and absence of different subclones during remission and relapses implies differing drug responses among subclones. Our study shows that time series analysis contrasting remission and relapse periods provides a much more comprehensive view of clonal structure and evolution.

摘要

大多数类型的癌症都是由遗传上不同的亚克隆组成的异质混合物。特别是,急性髓系白血病 (AML) 在疾病过程中已经被证明经历了大量的克隆进化。AML 往往比实体瘤具有更少的突变,因此难以推断克隆结构。在这里,我们在 12 个时间点对单个病例进行了长达 9 年的全外显子组测序研究,从最初的诊断到第四次复发,包括中间的 6 个缓解样本。据我们所知,这是同类数据集中时间跨度最长的数据集。我们使用这些时间序列数据来跟踪变异获得的层次结构和顺序,然后分析体细胞变异的进化来推断克隆结构。由此,我们假设亚克隆的发展和灭绝,以及它们通过不同的药物反应而相关的扩张。特别是,我们表明,在第一次完全缓解后,新的亚克隆开始出现。缓解期和复发期间不同亚克隆的存在和缺失意味着亚克隆之间存在不同的药物反应。我们的研究表明,对比缓解期和复发期的时间序列分析提供了对克隆结构和进化的更全面的了解。

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