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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Whole-genome sequencing of multiple myeloma from diagnosis to plasma cell leukemia reveals genomic initiating events, evolution, and clonal tides
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Whole-genome sequencing of multiple myeloma from diagnosis to plasma cell leukemia reveals genomic initiating events, evolution, and clonal tides

机译:从诊断到浆细胞白血病的多发性骨髓瘤的全基因组测序揭示了基因组启动事件,进化和克隆趋势

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The longitudinal evolution of a myeloma genome from diagnosis to plasma cell leukemia has not previously been reported. We used whole-genome sequencing (WGS) on 4 purified tumor samples and patient germline DNA drawn over a 5-year period in a t(4;14) multiple myeloma patient. Tumor samples were acquired at diagnosis, first relapse, second relapse, and end-stage secondary plasma cell leukemia (sPCL). In addition to the t(4;14), all tumor time points also shared 10 common single-nucleotide variants (SNVs) onWGScomprising shared initiating events. Interestingly, we observed genomic sequence variants that waxed and waned with time in progressive tumors, suggesting the presence of multiple independent, yet related, clones at diagnosis that rose and fell in dominance. Five newly acquired SNVs, including truncating mutations of RB1 and ZKSCAN3, were observed only in the final sPCL sample suggesting leukemic transformation events. This longitudinal WGS characterization of the natural history of a high-risk myeloma patient demonstrated tumor heterogeneity at diagnosis with shifting dominance of tumor clones over time and has also identified potential mutations contributing to myelomagenesis as well as transformation from myeloma to overt extramedullary disease such as sPCL.
机译:骨髓瘤基因组从诊断到浆细胞白血病的纵向进化先前尚未见报道。我们对t(4; 14)多发性骨髓瘤患者的5年内使用的4个纯化的肿瘤样品和患者种系DNA进行了全基因组测序(WGS)。在诊断,第一次复发,第二次复发和终末期继发性浆细胞白血病(sPCL)时采集肿瘤样本。除t(4; 14)外,所有肿瘤时间点在包含共享起始事件的WGS上还共享了10个常见的单核苷酸变体(SNV)。有趣的是,我们观察到了进行性肿瘤中随着时间的流逝而消逝的基因组序列变体,表明存在多个独立但相关的克隆,在诊断时占主导地位的上升和下降。仅在最终的sPCL样本中观察到五个新获得的SNV,包括RB1和ZKSCAN3的突变,提示存在白血病转化事件。对高危骨髓瘤患者的自然病史的这种纵向WGS表征显示出诊断时肿瘤异质性,随着时间的推移,肿瘤克隆的主导地位发生了变化,并且还鉴定了可能导致骨髓瘤形成的潜在突变,以及从骨髓瘤向明显的髓外疾病(如sPCL)的转化。

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