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Circulating tumor DNA analysis depicts subclonal architecture and genomic evolution of small cell lung cancer

机译:循环肿瘤DNA分析描述了小细胞肺癌的亚克隆结构和基因组进化

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摘要

Subclonal architecture and genomic evolution of small-cell lung cancer (SCLC) under treatment has not been well studied primarily due to lack of tumor specimens, particularly longitudinal samples acquired during treatment. SCLC is characterized by early hematogenous spread, which makes circulating cell-free tumor DNA (ctDNA) sequencing a promising modality for genomic profiling. Here, we perform targeted deep sequencing of 430 cancer genes on pre-treatment tumor biopsies, as well as on plasma samples collected prior to and during treatment from 22 SCLC patients. Similar subclonal architecture is observed between pre-treatment ctDNA and paired tumor DNA. Mean variant allele frequency of clonal mutations from pre-treatment ctDNA is associated with progression-free survival and overall survival. Pre- and post-treatment ctDNA mutational analysis demonstrate that mutations of DNA repair and NOTCH signaling pathways are enriched in post-treatment samples. These data suggest that ctDNA sequencing is promising to delineate genomic landscape, subclonal architecture, and genomic evolution of SCLC.
机译:主要由于缺乏肿瘤标本,特别是在治疗过程中获得的纵向样品,尚未对治疗中的小细胞肺癌(SCLC)的亚克隆结构和基因组进化进行深入研究。 SCLC的特征是早期血源性扩散,这使得循环的无细胞肿瘤DNA(ctDNA)测序成为基因组谱分析的有前途的方法。在这里,我们对治疗前的肿瘤活检以及治疗前和治疗期间从22位SCLC患者中收集的血浆样品进行了430个癌基因的靶向深度测序。在预处理ctDNA和配对的肿瘤DNA之间观察到相似的亚克隆结构。来自治疗前ctDNA的克隆突变的平均变异等位基因频率与无进展生存期和总体生存期相关。治疗前和治疗后ctDNA突变分析表明,治疗后样品中DNA修复和NOTCH信号通路的突变丰富。这些数据表明,ctDNA测序有望勾勒出SCLC的基因组图景,亚克隆结构和基因组进化。

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