首页> 美国卫生研究院文献>Haematologica >NOTCH1 mutations in +12 chronic lymphocytic leukemia (CLL) confer an unfavorable prognosis induce a distinctive transcriptional profiling and refine the intermediate prognosis of +12 CLL
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NOTCH1 mutations in +12 chronic lymphocytic leukemia (CLL) confer an unfavorable prognosis induce a distinctive transcriptional profiling and refine the intermediate prognosis of +12 CLL

机译:+12慢性淋巴细胞白血病(CLL)中的NOTCH1突变预后不良诱导独特的转录谱并改善+12 CLL的中间预后

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摘要

Trisomy 12, the third most frequent chromosomal aberration in chronic lymphocytic leukemia (CLL), confers an intermediate prognosis. In our cohort of 104 untreated patients carrying +12, NOTCH1 mutations occurred in 24% of cases and were associated to unmutated IGHV genes (P=0.003) and +12 as a sole cytogenetic abnormality (P=0.008). NOTCH1 mutations in +12 CLL associated with an approximately 2.4 fold increase in the risk of death, a significant shortening of survival (P<0.01) and proved to be an independent predictor of survival in multivariate analysis. Analogous to +12 CLL with TP53 disruption or del(11q), NOTCH1 mutations in +12 CLL conferred a significantly worse survival compared to that of +12 CLL with del(13q) or +12 only. The overrepresentation of cell cycle/proliferation related genes of +12 CLL with NOTCH1 mutations suggests the biological contribution of NOTCH1 mutations to determine a poor outcome. NOTCH1 mutations refine the intermediate prognosis of +12 CLL.
机译:在慢性淋巴细胞性白血病(CLL)中,第三体12号染色体畸变率第三高,可预示中等水平的预后。在我们的104名携带+12的未经治疗的患者队列中,NOTCH1突变发生在24%的病例中,并与未突变的IGHV基因相关(P = 0.003)和+12是唯一的细胞遗传学异常(P = 0.008)。 +12 CLL中的NOTCH1突变与死亡风险增加约2.4倍,生存时间显着缩短有关(P <0.01),并被证明是多变量分析中生存的独立预测因子。与带有TP53破坏或del(11q)的+12 CLL相似,与仅带有del(13q)或+12的+12 CLL相比,+ 12 CLL中的NOTCH1突变使存活率明显降低。带有NOTCH1突变的+12 CLL的细胞周期/增殖相关基因的过度表达表明,NOTCH1突变的生物学作用决定了不良结局。 NOTCH1突变改善了+12 CLL的中间预后。

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