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Methylation level of Rap1GAP and the clinical significance in MDS

机译:Rap1Gap的甲基化水平及MDS的临床意义

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摘要

Previous studies on the pathogenesis of myelodysplastic syndrome (MDS) have identified multiple associated gene mutations, including mutations of tetmethylcytosinedioxygenase 2, isocitrate dehydrogenase [NADP(+)] 1 cytosolic, isocitrate dehydrogenase [NADP(+)] 2 mitochondrial and additional sex combs like 1 transcriptional regulator, all of which may be considered epigenetic regulators. Furthermore, mutations of RAS type GTPase family genes have been identified in 10-15% patients with MDS. The authors' previous study on the gene expression profile of cluster of differentiation 34(+) cells using microarray analysis identified elevated expression of RAP1GTPase activating protein 1 (Rap1GAP) in patients with MDS compared with that in non-malignant blood diseases (NM) control group. To further investigate the mechanism of increased Rap1GAP expression, the methylation pattern of the promoter of this gene was determined in 86 patients with MDS (n=29), acute myeloid leukemia (AML) (n=31) or NM (n=26) using bisulfite-specific polymerase chain reaction and DNA sequencing. The results demonstrated that the methylation of Rap1GAP occurred in all 29 patients with MDS at multiple CpG sites. The methylation level of Rap1GAP in patients with MDS was decreased compared with that in patients with NM. Significant differences at 4CpG sites (5,7,8 and 12) of Rap1GAP promoter were identified between MDS and NM. Furthermore, based on the present clinical records of the patient cohort, the methylation status of Rap1GAP promoter did not appear to be associated with the clinicopathological characteristics of patients with MDS, including age, gender and International Prognosis Score System. The difference in methylation level at CpG site 8 of Rap1GAP promoter was identified to be significantly increased in patients with MDS-refractory anemia with ring sideroblasts compared with that in the MDS-refractory cytopenia with multilineage dysplasia or MDS-unclassified groups. The results of the present study suggest that patients with MDS exhibit a lower overall methylation level within Rap1GAP promoter compared with patients with NM or AML. In addition, the methylation level at the four identified CpG sites can distinguish between MDS and NM.
机译:以前关于髓细胞增强型综合征(MDS)发病机制的研究已经确定了多种相关的基因突变,包括TetmethylyliOniOxygenase 2的突变,异柠檬酸脱氢酶[NADP(+)] 1个细胞溶质,异柠檬酸脱氢酶[NADP(+)] 2线粒体和额外的性梳1转录调节剂,所有这些调节剂可能被认为是表观遗传调节因子。此外,已经在10-15%的MDS患者中鉴定了RAS型GTPase家族基因的突变。使用微阵列分析的分化34(+)细胞簇基因表达谱的基因表达谱的研究确定了与非恶性血液疾病(NM)对照相比,MDS患者Rap1gTPase活化蛋白1(Rap1Gap)的表达升高团体。为了进一步研究增加的Rap1Gap表达的机制,在86例MDS(n = 29),急性髓性白血病(AML)(n = 31)或Nm(n = 26)中,测定该基因启动子的甲基化模式。(n = 31)使用亚硫酸氢盐特异性聚合酶链反应和DNA测序。结果表明,RAP1GAP的甲基化在多个CPG位点的所有29例MDS患者中发生。与NM患者相比,MDS患者Rap1Gap的甲基化水平降低。在MDS和NM之间鉴定出Rap1Gap启动子的4cpg位点(5,7,8和12)的显着差异。此外,基于患者队列的本临床记录,RAP1GAP启动子的甲基化状态似乎与MDS患者的临床病理特征有关,包括年龄,性别和国际预测分数系统。鉴定RAP1GAP启动子CPG部位8的甲基化水平的差异在具有环状血管血细胞的MDS-难治性贫血患者中显着增加,与MDS-难治性细胞质细胞增多细胞增多细胞增生,具有多线性发育性或未分类基团。本研究结果表明,与NM或AML患者相比,MDS患者在RAP1GAP启动子中表现出较低的总甲基化水平。另外,四个鉴定的CPG位点的甲基化水平可以区分MDS和NM。

著录项

  • 来源
    《Oncology letters 》 |2018年第6期| 共8页
  • 作者单位

    Soochow Univ Affiliated Hosp 1 Jiangsu Inst Hematol Key Lab Thrombosis &

    Hemostasis Minist Hlth;

    Soochow Univ Affiliated Hosp 1 Jiangsu Inst Hematol Key Lab Thrombosis &

    Hemostasis Minist Hlth;

    Soochow Univ Affiliated Hosp 1 Jiangsu Inst Hematol Key Lab Thrombosis &

    Hemostasis Minist Hlth;

    Soochow Univ Affiliated Hosp 1 Jiangsu Inst Hematol Key Lab Thrombosis &

    Hemostasis Minist Hlth;

    Soochow Univ Affiliated Hosp 1 Jiangsu Inst Hematol Key Lab Thrombosis &

    Hemostasis Minist Hlth;

    Soochow Univ Affiliated Hosp 1 Jiangsu Inst Hematol Key Lab Thrombosis &

    Hemostasis Minist Hlth;

    Soochow Univ Affiliated Hosp 1 Jiangsu Inst Hematol Key Lab Thrombosis &

    Hemostasis Minist Hlth;

    Soochow Univ Affiliated Hosp 1 Jiangsu Inst Hematol Key Lab Thrombosis &

    Hemostasis Minist Hlth;

    Soochow Univ Affiliated Hosp 1 Jiangsu Inst Hematol Key Lab Thrombosis &

    Hemostasis Minist Hlth;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 肿瘤学 ;
  • 关键词

    myelodysplastic syndrome; RAP1GTPase activating protein 1 methylation level;

    机译:髓细胞增生综合征;RAP1GTPase激活蛋白1甲基化水平;

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