Methylation and Expression Status of The CpG-Island of SMG1 Promoter in Acute Myeloid Leukemia: A Follow-Up Study in Patients

Neda Karami, M. Ahmadi, S. Mohammadi, Amirhosein Maali, A. Alizadeh, Shaghayegh Pishkhan Dibazar, M. Azad
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Abstract

Objective Aberrant alterations in DNA methylation are known as one of the hallmarks of oncogenesis and play a vital role in the progression of acute myeloid leukemia (AML). SMG1 is a member of the Phosphoinositide 3-kinases family, acting as a tumor suppressor gene. The aim of this study was the evaluation of the expression level and methylation status of SMG1 in AML. Materials and Methods In this follow-up study on AML patients admitted to Shariati Hospital, Tehran, Iran, the methylation status of SMG1 [performed by methylation-specific polymerase chain reaction (PCR)] and its expression level (performed by qRT-PCR) were evaluated in three phases: newly diagnosed, under treatment and complete remission. The correlation of the methylation status of SMG1, its expression level, and clinical/paraclinical data was analyzed by SPSS ver.25. Results This study on 18 patients and five control individuals showed that the CpG-islands of the SMG1 promoter in newly diagnosed cases is hypomethylated compared to the normal group (P=0.002) The fold change of SMG1 expression levels in new cases is 0.464 ± 0.468, while the fold change of SMG1 expression levels in under-treatment and in-remission patients is 0.973 ± 1.159 and 0.685 ± 0.885, respectively. In under-treatment patients, white blood cell (WBC) count decreases 114176.36 cell/µl with each unit of increase in fold change of SMG1 (P<0.0001), and Hb unit increases 2.062 g/dl with each unit of increase in fold change (P<0.0001) Also, in the remission phase, the Hb unit increases 1.395 g/dl with each unit increase in fold change (P=0.019). Conclusion The robust results of our study suggest that the methylation and expression of have a high impact on the pathogenesis of AML. Also, the methylation and expression of SMG1 can play a prognostic role in AML.
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急性髓系白血病患者SMG1启动子cpg岛甲基化及表达状态:一项随访研究
DNA甲基化的异常改变是肿瘤发生的标志之一,在急性髓性白血病(AML)的进展中起着至关重要的作用。SMG1是磷酸肌苷3激酶家族的成员,作为肿瘤抑制基因。本研究的目的是评估AML中SMG1的表达水平和甲基化状态。材料与方法本研究对伊朗德黑兰Shariati医院住院的AML患者进行随访研究,将SMG1的甲基化状态[采用甲基化特异性聚合酶链反应(methyl- specific polymerase chain reaction, PCR)]和表达水平(采用qRT-PCR)分为新诊断、正在治疗和完全缓解三个阶段进行评估。采用SPSS ver.25分析SMG1甲基化状态及其表达水平与临床/临床旁数据的相关性。结果18例患者和5例对照患者的研究结果显示,新发病例中SMG1启动子cpg岛较正常组低甲基化(P=0.002),新发病例中SMG1表达水平的翻倍变化为0.464±0.468,治疗不足和缓解期患者中SMG1表达水平的翻倍变化分别为0.973±1.159和0.685±0.885。在治疗不足的患者中,随着SMG1倍数变化每增加一个单位,白细胞(WBC)计数减少114176.36个细胞/µl (P<0.0001),随着SMG1倍数变化每增加一个单位,Hb单位增加2.062 g/dl (P<0.0001)。在缓解期,随着SMG1倍数变化每增加一个单位,Hb单位增加1.395 g/dl (P=0.019)。结论我们的研究结果表明,甲基化和表达对AML的发病机制有重要影响。此外,SMG1的甲基化和表达可以在AML中发挥预后作用。
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