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Evolution of multiple cell clones over a 29-year period of a CLL patient

机译:CLL患者29年内多个细胞克隆的进化

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Chronic lymphocytic leukaemia (CLL) is a frequent B-cell malignancy, characterized by recurrent somatic chromosome alterations and a low level of point mutations. Here we present single-nucleotide polymorphism microarray analyses of a single CLL patient over 29 years of observation and treatment, and transcriptome and whole-genome sequencing at selected time points. We identify chromosome alterations 13q14?, 6q? and 12q+ in early cell clones, elimination of clonal populations following therapy, and subsequent appearance of a clone containing trisomy 12 and chromosome 10 copy-neutral loss of heterogeneity that marks a major population dominant at death. Serial single-cell RNA sequencing reveals an expression pattern with high FOS , JUN and KLF4 at disease acceleration, which resolves following therapy, but reoccurs following relapse and death. Transcriptome evolution indicates complex changes in expression occur over time. In conclusion, CLL can evolve gradually during indolent phases, and undergo rapid changes following therapy.
机译:慢性淋巴细胞性白血病(CLL)是一种常见的B细胞恶性肿瘤,其特征是复发性体细胞染色体改变和低水平的点突变。在这里,我们介绍了在29年的观察和治疗中对一名CLL患者的单核苷酸多态性微阵列分析,以及在选定时间点的转录组和全基因组测序。我们确定染色体改变13q14?,6q?早期细胞克隆中的12q +和12q +,在治疗后消除了克隆种群,随后出现了包含三体性12和染色体10复制中性非均质性丧失的克隆,这标志着主要种群在死亡时占优势。连续单细胞RNA测序揭示了在疾病加速时具有高FOS,JUN和KLF4的表达模式,该模式在治疗后可解决,但在复发和死亡后会再次出现。转录组进化表明表达随时间发生复杂变化。总之,CLL可在惰性期逐渐发展,并在治疗后发生快速变化。

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