[半胱天冬酶8关联蛋白2基因甲基化在儿童急性淋巴细胞白血病中的临床意义]
[Clinical significance of CASP8AP2 gene methylation in childhood acute lymphoblastic leukemia].
作者信息
Liu Fei-Fei, Liu Xiao, Wang Kai-Ling, Li Wei-Jing, Deng Guo-Ren, Gao Chao, Zhao Xiao-Xi, Wu Min-Yuan, Cui Lei, Li Zhi-Gang
机构信息
Hematologic Oncology Center, Beijing Children's Hospital, Capital Medical University; Key Laboratory of Major Diseases in Children, Ministry of Education; National Key Discipline of Pediatrics; Beijing Key Laboratory of Pediatric Hematology and Oncology; Beijing 100045, China.
Department of Urology, School of Medicine, University of California, San Francisco, CA 94101, USA.
出版信息
Zhongguo Shi Yan Xue Ye Xue Za Zhi. 2015 Feb;23(1):6-11. doi: 10.7534/j.issn.1009-2137.2015.01.002.
OBJECTIVE
To study the methylation level in the promoter of caspase 8 associated protein 2 (CASP8AP2) gene between samples at diagnosis and in complete remission, and to investigate its relationship with clinical features and prognosis in children with acute lymphoblastic leukemia (ALL).
METHODS
Diagnostic DNA samples from 109 newly diagnosed children with ALL admitted from August 2007 to March 2010, and 94 ALL children in CR (complete remission) among them were collected. Bisulfite modification and MethyLight method established by our research team were used to determine the methylation level of the two key CpG sites (at -1189 and -1176) of the promoter of CASP8AP2 gene.
RESULTS
The average methylation level of the two CpG sites in newly diagnosted samples was higher than that in CR samples (71.1% ± 1.7% vs 64.2% ± 21.2%) (P = 0.008). Analysis with receiver operating characteristic (ROC) curve showed that the area under curve was 0.687 (P = 0.024), indicating that the methylation level of the two CpG sites was able to predict relapse efficiently to some extent, 76.9% was chosed as a cutoff value to divide the patients into high methylation group (49 patients) and low methylation group (60 patients). The incidence of relapse in high methylation group was higher than that in low methylation group (20.4% vs 6.7%) (P = 0.044), five year relapse free survival in high methylation group was also lower than that in low methylation group (Log rank, P = 0.033). Furthermore, high methylation at new diagnosis were correlated with high level of minimal residual disease (MRD) before consolidation therapy (P = 0.011). In the 34 children with MRD ≥ 10(-4) at the end of induction remission, the relapse rate of high methylation patients was significantly higher than that of low methylation patients (8/16 vs 3/18)(P = 0.038).
CONCLUSION
The abnormal hypermethylation of the two CpG sites (at -1189 and -1176) of the promoter of the CASP8AP2 gene is possibly associated with leukemogenesis in childhood ALL. The treatment outcome is more poor in patients with hypermethylation than that in patients with low methylation. The combination of the methylation level of the two CpG sites and MRD level at the end induction remission is able to predict relapse more effectively.
目的
研究急性淋巴细胞白血病(ALL)患儿诊断时与完全缓解期样本中半胱天冬酶8相关蛋白2(CASP8AP2)基因启动子的甲基化水平,并探讨其与临床特征及预后的关系。
方法
收集2007年8月至2010年3月收治的109例新诊断ALL患儿的诊断时DNA样本,其中94例处于完全缓解(CR)期的ALL患儿。采用本研究团队建立的亚硫酸氢盐修饰和MethyLight方法,测定CASP8AP2基因启动子两个关键CpG位点(-1189和-1176处)的甲基化水平。
结果
新诊断样本中两个CpG位点的平均甲基化水平高于CR样本(71.1%±1.7%对64.2%±21.2%)(P = 0.008)。通过受试者工作特征(ROC)曲线分析显示,曲线下面积为0.687(P = 0.024),表明两个CpG位点的甲基化水平在一定程度上能够有效预测复发,选取76.9%作为临界值将患者分为高甲基化组(49例)和低甲基化组(60例)。高甲基化组的复发率高于低甲基化组(20.4%对6.7%)(P = 0.044),高甲基化组的5年无复发生存率也低于低甲基化组(Log秩检验,P = 0.033)。此外,新诊断时高甲基化与巩固治疗前微小残留病(MRD)水平高相关(P = 0.011)。在诱导缓解期末MRD≥10⁻⁴的34例患儿中,高甲基化患者的复发率显著高于低甲基化患者(8/16对3/18)(P = 0.038)。
结论
CASP8AP2基因启动子两个CpG位点(-1189和-1176处)的异常高甲基化可能与儿童ALL的白血病发生有关。高甲基化患者的治疗结局比低甲基化患者更差。两个CpG位点的甲基化水平与诱导缓解期末MRD水平相结合能够更有效地预测复发。
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