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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Clonal origins of relapse in ETV6-RUNX1 acute lymphoblastic leukemia.
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Clonal origins of relapse in ETV6-RUNX1 acute lymphoblastic leukemia.

机译:ETV6-RUNX1急性淋巴细胞白血病复发的克隆起源。

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B-cell precursor childhood acute lymphoblastic leukemia with ETV6-RUNX1 (TEL-AML1) fusion has an overall good prognosis, but relapses occur, usually after cessation of treatment and occasionally many years later. We have investigated the clonal origins of relapse by comparing the profiles of genomewide copy number alterations at presentation in 21 patients with those in matched relapse (12-119 months). We identified, in total, 159 copy number alterations at presentation and 231 at relapse (excluding Ig/TCR). Deletions of CDKN2A/B or CCNC (6q16.2-3) or both increased from 38% at presentation to 76% in relapse, suggesting that cell-cycle deregulation contributed to emergence of relapse. A novel observation was recurrent gain of chromosome 16 (2 patients at presentation, 4 at relapse) and deletion of plasmocytoma variant translocation 1 in 3 patients. The data indicate that, irrespective of time to relapse, the relapse clone was derived from either a major or minor clone at presentation. Backtracking analysis by FISH identified a minor subclone at diagnosis whose genotype matched that observed in relapse approximately 10 years later. These data indicate subclonal diversity at diagnosis, providing a variable basis for intraclonal origins of relapse and extended periods (years) of dormancy, possibly by quiescence, for stem cells in ETV6-RUNX1(+) acute lymphoblastic leukemia.
机译:具有ETV6-RUNX1(TEL-AML1)融合的B细胞前体儿童期急性淋巴细胞白血病具有总体良好的预后,但通常会在治疗停止后以及很多年后复发。我们通过比较21例与匹配复发(12-119个月)的患者的全基因组拷贝数变化情况,研究了复发的克隆起源。我们总共发现了159份拷贝数变化和231份复发(不包括Ig / TCR)。 CDKN2A / B或CCNC(6q16.2-3)或两者的缺失从呈报时的38%增加到复发时的76%,表明细胞周期失调导致了复发的出现。一项新的观察结果是,复发性增加了16号染色体(在诊2例,复发4例)和3例浆细胞瘤变体易位1缺失。数据表明,无论复发时间如何,复发克隆都来自出现时的主要或次要克隆。 FISH的回溯分析在诊断时发现了一个较小的亚克隆,其基因型与大约10年后复发中观察到的基因型相匹配。这些数据表明诊断时亚克隆的多样性,为ETV6-RUNX1(+)急性淋巴细胞白血病干细胞的复发和延长的休眠期(年)(可能通过休眠)提供了可变的基础。

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