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成人急性髓系白血病中预后预测基因及新型分子分类方案

Genes predictive of outcome and novel molecular classification schemes in adult acute myeloid leukemia.

作者信息

Verhaak Roel G W, Valk Peter J M

机构信息

Department of Hematology, Erasmus University Medical Center, Rotterdam, The Netherlands.

出版信息

Cancer Treat Res. 2010;145:67-83. doi: 10.1007/978-0-387-69259-3_5.

DOI:10.1007/978-0-387-69259-3_5
PMID:20306246
Abstract

The pretreatment karyotype of leukemic blasts is currently the key determinant in therapy decision making in acute myeloid leukemia (AML). The World Health Organization (WHO) has recognized this important information by including, besides clinical, cytological, cytochemical, and immunophenotypical features, recurrent cytogenetic abnormalities in its classification (Table 1). However, although the WHO defines important biologically and clinically relevant entities, the prognostic value of some of the well-defined cytogenetic subgroups is partially masked in the WHO classification. Moreover, in the recent past a number of novel molecular aberrations with marked prognostic value, which are not yet incorporated in the WHO classifications have been identified. These molecular abnormalities include mutations (e.g., in FLT3, c-KIT, and NPM1), partial duplications (e.g., of MLL and FLT3), and abnormal expression of pathogenetic genes (e.g., EVI1, WT1, BCL2, MDR1, BAALC, and ERG). In addition, novel molecular approaches in genomics, like monitoring the expression levels of thousands of genes in parallel using DNA microarray technology, open possibilities for further refinement of prognostication of AML. Gene expression profiling in AML is already well established and has proven to be valuable to recognize various cytogenetic subtypes, discover novel AML subclasses, and predict clinical outcome. The current advances made in molecular understanding of AML will ultimately lead to a further refinement of prognostics of AML.

摘要

白血病原始细胞的预处理核型目前是急性髓系白血病(AML)治疗决策的关键决定因素。世界卫生组织(WHO)已认识到这一重要信息,除了临床、细胞学、细胞化学和免疫表型特征外,还将复发性细胞遗传学异常纳入其分类中(表1)。然而,尽管WHO定义了重要的生物学和临床相关实体,但在WHO分类中,一些明确的细胞遗传学亚组的预后价值部分被掩盖。此外,最近还发现了一些具有显著预后价值的新型分子异常,但尚未纳入WHO分类中。这些分子异常包括突变(如FLT3、c-KIT和NPM1中的突变)、部分重复(如MLL和FLT3的重复)以及致病基因的异常表达(如EVI1、WT1、BCL2、MDR1、BAALC和ERG)。此外,基因组学中的新型分子方法,如使用DNA微阵列技术并行监测数千个基因的表达水平,为进一步完善AML的预后评估开辟了可能性。AML中的基因表达谱分析已经成熟,并已证明对于识别各种细胞遗传学亚型、发现新型AML亚类以及预测临床结果具有重要价值。目前在AML分子理解方面取得的进展最终将导致AML预后评估的进一步完善。

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