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一组调节细胞增殖的基因可预测儿童急性淋巴细胞白血病的治疗结果。

A set of genes that regulate cell proliferation predicts treatment outcome in childhood acute lymphoblastic leukemia.

作者信息

Flotho Christian, Coustan-Smith Elaine, Pei Deqing, Cheng Cheng, Song Guangchun, Pui Ching-Hon, Downing James R, Campana Dario

机构信息

Departments of Pathology, St Jude Children's Research Hospital, Memphis, TN 38105, USA.

出版信息

Blood. 2007 Aug 15;110(4):1271-7. doi: 10.1182/blood-2007-01-068478. Epub 2007 Apr 24.

Abstract

To identify novel predictors of outcome in childhood acute lymphoblastic leukemia (ALL), we analyzed gene expression in the leukemic cells of 187 children with newly diagnosed ALL and compared the findings with minimal residual disease (MRD) results obtained on day 19 of remission induction treatment. Genes that showed a significant relationship to MRD were then tested for their capacity to predict leukemic relapse in an independent cohort of 99 patients. We identified 674 probe sets that were associated with MRD on day 19 (P < .006); 40 of the identified genes predicted relapse (P < .03). Among these, 14 showed independent prognostic significance after adjustment for age, leukocyte count at diagnosis, and genetic subtype. More than half of the 40 genes and nearly all of the 14 genes were functionally related, as indicated by their roles in the regulation of cell proliferation. Underexpression of genes promoting cell proliferation was associated with resistance to chemotherapy. The biologic processes regulated by the genes we identified appear to be key determinants of the early cytoreductive response to remission induction therapy and subsequent clinical outcome in childhood ALL. Incorporation of the expression levels of these genes into existing strategies of risk classification could improve clinical management.

摘要

为了确定儿童急性淋巴细胞白血病(ALL)预后的新预测指标,我们分析了187例新诊断ALL患儿白血病细胞中的基因表达,并将结果与缓解诱导治疗第19天获得的微小残留病(MRD)结果进行比较。然后在一个由99例患者组成的独立队列中测试与MRD有显著关系的基因预测白血病复发的能力。我们鉴定出674个与第19天MRD相关的探针组(P <.006);鉴定出的40个基因可预测复发(P <.03)。其中,14个基因在调整年龄、诊断时白细胞计数和基因亚型后显示出独立的预后意义。40个基因中的一半以上以及14个基因中的几乎所有基因在功能上相关,这可从它们在细胞增殖调节中的作用看出。促进细胞增殖的基因低表达与化疗耐药相关。我们鉴定出的基因所调控的生物学过程似乎是儿童ALL早期对缓解诱导治疗的细胞减少反应及后续临床结果的关键决定因素。将这些基因的表达水平纳入现有的风险分类策略中可改善临床管理。

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