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Clinical impact of the subclonal architecture and mutational complexity in chronic lymphocytic leukemia

机译:慢性淋巴细胞白血病亚克隆结构和突变复杂性的临床影响

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摘要

Genome studies of chronic lymphocytic leukemia (CLL) have revealed the remarkable subclonal heterogeneity of the tumors, but the clinical implications of this phenomenon are not well known. We assessed the mutational status of 28 CLL driver genes by deep-targeted next-generation sequencing and copy number alterations (CNA) in 406 previously untreated patients and 48 sequential samples. We detected small subclonal mutations (0.6–25% of cells) in nearly all genes (26/28), and they were the sole alteration in 22% of the mutated cases. CNA tended to be acquired early in the evolution of the disease and remained stable, whereas the mutational heterogeneity increased in a subset of tumors. The prognostic impact of different genes was related to the size of the mutated clone. Combining mutations and CNA, we observed that the accumulation of driver alterations (mutational complexity) gradually shortened the time to first treatment independently of the clonal architecture, IGHV status and Binet stage. Conversely, the overall survival was associated with the increasing subclonal diversity of the tumors but it was related to the age of patients, IGHV and TP53 status of the tumors. In conclusion, our study reveals that both the mutational complexity and subclonal diversity influence the evolution of CLL.
机译:慢性淋巴细胞性白血病(CLL)的基因组研究表明,肿瘤具有显着的亚克隆异质性,但是这种现象的临床意义尚不明确。我们通过深度靶向的下一代测序和拷贝数改变(CNA)在406位先前未接受治疗的患者和48位连续样本中评估了28个CLL驱动基因的突变状态。我们在几乎所有基因(26/28)中检测到小的亚克隆突变(占细胞的0.6–25%),而在22%的突变病例中,它们是唯一的改变。 CNA倾向于在疾病发展的早期获得,并保持稳定,而突变异质性在一部分肿瘤中增加。不同基因的预后影响与突变克隆的大小有关。结合突变和CNA,我们观察到驱动程序改变(突变复杂性)的积累逐渐缩短了首次治疗的时间,而与克隆结构,IGHV状态和Binet阶段无关。相反,总体存活与肿瘤亚克隆多样性的增加有关,但与患者的年龄,IGHV和肿瘤的TP53状态有关。总之,我们的研究表明突变复杂性和亚克隆多样性都影响CLL的进化。

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