治疗相关性急性髓系白血病的细胞遗传学和遗传学途径。
Cytogenetic and genetic pathways in therapy-related acute myeloid leukemia.
机构信息
Section of Hematology/Oncology, Department of Medicine and the Cancer Research Center, University of Chicago, 5841 S Maryland Ave, MC2115, Chicago, IL 60637, USA.
出版信息
Chem Biol Interact. 2010 Mar 19;184(1-2):50-7. doi: 10.1016/j.cbi.2009.11.025. Epub 2009 Dec 1.
Therapy-related myelodysplastic syndrome and acute myeloid leukemia (t-MDS/t-AML) are late complications of cytotoxic therapy used in the treatment of malignant diseases. The most common subtype of t-AML ( approximately 75% of cases) develops after exposure to alkylating agents, and is characterized by loss or deletion of chromosome 5 and/or 7 [-5/del(5q), -7/del(7q)], and a poor outcome (median survival 8 months). In the University of Chicago's series of 386 patients with t-MDS/t-AML, 79 (20%) patients had abnormalities of chromosome 5, 95 (25%) patients had abnormalities of chromosome 7, and 85 (22%) patients had abnormalities of both chromosomes 5 and 7. t-MDS/t-AML with a -5/del(5q) is associated with a complex karyotype, characterized by trisomy 8, as well as loss of 12p, 13q, 16q22, 17p (TP53 locus), chromosome 18, and 20q. In addition, this subtype of t-AML is characterized by a unique expression profile (higher expression of genes) involved in cell cycle control (CCNA2, CCNE2, CDC2), checkpoints (BUB1), or growth (MYC), loss of expression of IRF8, and overexpression of FHL2. Haploinsufficiency of the RPS14, EGR1, APC, NPM1, and CTNNA1 genes on 5q has been implicated in the pathogenesis of MDS/AML. In previous studies, we determined that Egr1 acts by haploinsufficiency and cooperates with mutations induced by alkylating agents to induce myeloid leukemias in the mouse. To identify mutations that cooperate with Egr1 haploinsufficiency, we used retroviral insertional mutagenesis. To date, we have identified two common integration sites involving genes encoding transcription factors that play a critical role in hematopoiesis (Evi1 and Gfi1b loci). Of note is that the EVI1 transcription factor gene is deregulated in human AMLs, particularly those with -7, and abnormalities of 3q. Identifying the genetic pathways leading to t-AML will provide new insights into the underlying biology of this disease, and may facilitate the identification of new therapeutic targets.
治疗相关骨髓增生异常综合征和急性髓系白血病(t-MDS/t-AML)是恶性疾病治疗中使用细胞毒性疗法的晚期并发症。t-AML 最常见的亚型(约 75%的病例)在接触烷化剂后发展而来,其特征是染色体 5 和/或 7 的缺失或丢失[-5/del(5q),-7/del(7q)],且预后不良(中位生存期 8 个月)。在芝加哥大学的 386 例 t-MDS/t-AML 患者中,79 例(20%)患者存在染色体 5 异常,95 例(25%)患者存在染色体 7 异常,85 例(22%)患者同时存在染色体 5 和 7 异常。t-MDS/t-AML 伴 -5/del(5q)与复杂核型相关,其特征是三体 8,以及 12p、13q、16q22、17p(TP53 基因座)、18 号染色体和 20q 的缺失。此外,这种 t-AML 亚型的特征是独特的表达谱(细胞周期控制相关基因的表达升高,如 CCNA2、CCNE2、CDC2)、检查点(BUB1)或生长(MYC),IRF8 表达缺失,FHL2 过表达。5q 上的 RPS14、EGR1、APC、NPM1 和 CTNNA1 基因的单倍体不足与 MDS/AML 的发病机制有关。在之前的研究中,我们确定 Egr1 通过单倍体不足起作用,并与烷化剂诱导的突变协同诱导小鼠发生髓系白血病。为了鉴定与 Egr1 单倍体不足协同作用的突变,我们使用了逆转录病毒插入诱变。迄今为止,我们已经确定了两个常见的整合位点,涉及在造血中发挥关键作用的转录因子基因(Evi1 和 Gfi1b 基因座)。值得注意的是,EVI1 转录因子基因在人类 AML 中失调,特别是那些具有 -7 和 3q 异常的 AML。鉴定导致 t-AML 的遗传途径将为该疾病的基础生物学提供新的见解,并可能有助于鉴定新的治疗靶点。
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