Expression of deubiquitinase genes and inflammatory response in myeloid leukemia

Nguyen Thi Thanh Huyen, Nguyen Hoang Giang, Nguyen Thi Xuan
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Abstract

Myeloid leukemia (ML) is a cancer of the blood that begins when cells of the myeloid lineage uncontrollably change and grow. Acute myeloid leukemia (AML) is a disorder of rapid, uncontrolled growth of immature myeloid cells in the blood and bone marrow. Chronic myeloid leukemia (CML) is characterized by the aberrant proliferation of myeloid cells and driven by the translocation of regions of the BCR and ABL genes to form the Philadelphia (Ph) chromosome. The deubiquitinase enzymes (DUBs) including A20, OTUB1, OTUB2, and Cezanne play important roles in inhibiting NF-κB activation in response to various stimuli. Cytokines including tumor necrosis factor-alpha (TNF-α), IL-6, and IL-1β are released from immune cell activation triggered by antigenic stimulation. To this end, blood samples of 20 AML and 62 CML patients and the control group consisting of 37 healthy individuals were used to examine the mRNA expression of A20, OTUB1, OTUB2 and Cezanne genes by using quantitative RT-PCR and determine IL-6, TNF-α and IL-1β concentrations by using ELISA. As a result, the mRNA level of OTUB1 was significantly decreased in both AML and CML patients compared to that in healthy individuals, however, no difference in the transcriptional expression of OTUB2 among AML and CML patients and control group was detected. Unlike the levels of OTUB1 and OTUB2, the expressions of A20 and Cezanne in CML, but not in AML patients were significantly lower than healthy individuals. For serum cytokine analysis of the study groups, in AML and CML samples, IL-6 and TNF-α concentrations significantly increased in comparison with the control group, however, IL-1β level was similar among CML, AML patients and healthy individuals. In conclusion, this study revealed the different DUB involvement in the pathogenesis of ML, suggesting further investigations on gene polymorphisms and their functions linked to biological properties of leukemia cells.
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去泛素酶基因在髓性白血病中的表达与炎症反应
髓系白血病(ML)是一种血液癌症,起源于髓系细胞不受控制的变化和生长。急性髓性白血病(AML)是一种未成熟髓细胞在血液和骨髓中快速、不受控制地生长的疾病。慢性髓细胞白血病(CML)的特点是髓细胞异常增殖,并由BCR和ABL基因区域易位驱动形成费城(Ph)染色体。deubiquitinase (DUBs)包括A20、OTUB1、OTUB2和Cezanne等,在各种刺激下抑制NF-κB的活化中发挥重要作用。包括肿瘤坏死因子-α (TNF-α)、IL-6和IL-1β在内的细胞因子是由抗原刺激触发的免疫细胞激活释放的。为此,采用定量RT-PCR检测20例AML和62例CML患者及37例健康对照组的A20、OTUB1、OTUB2和塞尚基因mRNA表达,ELISA检测IL-6、TNF-α和IL-1β浓度。结果,AML和CML患者中OTUB1 mRNA水平与健康人群相比均显著降低,而OTUB2转录表达在AML和CML患者与对照组中未见差异。与OTUB1和OTUB2的表达水平不同,A20和Cezanne在CML中的表达明显低于健康个体,而在AML患者中没有。对于研究组的血清细胞因子分析,在AML和CML样本中,IL-6和TNF-α浓度与对照组相比显著升高,而IL-1β水平在CML、AML患者和健康个体中相似。总之,本研究揭示了不同的DUB参与ML的发病机制,提示进一步研究与白血病细胞生物学特性相关的基因多态性及其功能。
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