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中期核型分析检测到的克隆异质性是急性髓系白血病预后不良的指标。

Clonal heterogeneity as detected by metaphase karyotyping is an indicator of poor prognosis in acute myeloid leukemia.

机构信息

Tilmann Bochtler, Christoph E. Heilig, Anna Jauch, Johannes W.G. Janssen, Anthony D. Ho, and Alwin Krämer, University of Heidelberg; Tilmann Bochtler, Christina Kunz, Axel Benner, and Alwin Krämer, German Cancer Research Center (DKFZ), Heidelberg; and Friedrich Stölzel, Brigitte Mohr, Michael Kramer, Martin Bornhäuser, Gerhard Ehninger, and Markus Schaich, University Hospital Carl Gustav Carus, Dresden, Germany.

出版信息

J Clin Oncol. 2013 Nov 1;31(31):3898-905. doi: 10.1200/JCO.2013.50.7921. Epub 2013 Sep 23.

Abstract

PURPOSE

In acute myeloid leukemia (AML), studies based on whole-genome sequencing have shown genomic diversity within leukemic clones. The aim of this study was to address clonal heterogeneity in AML based on metaphase cytogenetics.

PATIENTS AND METHODS

This analysis included all patients enrolled onto two consecutive, prospective, randomized multicenter trials of the Study Alliance Leukemia. Patients were newly diagnosed with non-M3 AML and were fit for intensive chemotherapy.

RESULTS

Cytogenetic subclones were detected in 418 (15.8%) of 2,639 patients from the whole study population and in 418 (32.8%) of 1,274 patients with aberrant karyotypes. Among those, 252 karyotypes (60.3%) displayed a defined number of distinct subclones, and 166 (39.7%) were classified as composite karyotypes. Subclone formation was particularly frequent in the cytogenetically adverse group, with subclone formation in 69.0%, 67.1%, and 64.8% of patients with complex aberrant, monosomal, and abnl(17p) karyotypes (P < .001 each). Two-subclone patterns typically followed a mother-daughter evolution, whereas for ≥ three subclones, a branched pattern prevailed. In non-core binding factor AML, subclone formation was associated with inferior event-free and overall survival and was confirmed as an independent predictor of poor prognosis in multivariate analysis. Subgroup analysis showed that subclone formation adds prognostic information particularly in the cytogenetic adverse-risk group. Allogeneic stem-cell transplantation improved the prognosis of patients with subclone karyotypes as shown in landmark analyses.

CONCLUSION

Cytogenetic subclones are frequent in AML and permit tracing of clonal evolution and architecture. They bear prognostic significance with clonal heterogeneity as an independent adverse prognostic marker in cytogenetically adverse-risk AML.

摘要

目的

在急性髓系白血病(AML)中,基于全基因组测序的研究表明白血病克隆内存在基因组多样性。本研究旨在基于中期细胞遗传学探讨 AML 中的克隆异质性。

患者和方法

该分析纳入了 Study Alliance Leukemia 两项连续前瞻性随机多中心试验中所有入组的患者。患者新诊断为非 M3 AML,适合强化化疗。

结果

在整个研究人群的 2639 例患者和核型异常的 1274 例患者中,分别检测到 418 例(15.8%)和 418 例(32.8%)细胞遗传学亚克隆。其中,252 个核型(60.3%)显示出明确数量的不同亚克隆,166 个核型(39.7%)被归类为复合核型。亚克隆形成在细胞遗传学不良组中尤为常见,复杂异常、单体和 abnl(17p)核型患者的亚克隆形成率分别为 69.0%、67.1%和 64.8%(均<.001)。二亚克隆模式通常遵循母子进化,而对于≥三个亚克隆,分支模式占主导地位。在非核心结合因子 AML 中,亚克隆形成与无事件生存和总生存不良相关,并在多变量分析中被证实为预后不良的独立预测因子。亚组分析表明,亚克隆形成在细胞遗传学不良风险组中尤其提供了预后信息。在标志分析中,异基因造血干细胞移植改善了具有亚克隆核型患者的预后。

结论

细胞遗传学亚克隆在 AML 中很常见,可追踪克隆进化和结构。它们具有预后意义,作为细胞遗传学不良风险 AML 中的独立不良预后标志物,克隆异质性具有预后意义。

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