伊拉克hcv暴露患者血清NF-kB水平与microrna-221表达模式的相关性

Shaima’a R. Al-Salihy, R. Al-Shawk, Safaa A. Al-Waysi, M. Rasheed
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Materials and Methods: Serum level of NF-κB in 88 samples (22 patients with persistent HCV infection, 22 individuals with spontaneous HCV virus clearance, 22 individuals treated with direct-acting antivirals (DAAs) drugs, and 22 uninfected apparently healthy blood donors as control) was measured by enzyme-linked immunosorbent assay. Reverse transcriptase–polymerase chain reaction was used to quantify the expression fold of circulatory miR-221. Results: The results showed that there was a significant decrease in the mean level of NF-κB at P < 0.000 among HCV-exposed patients (2.0058 ng/ml) as compared to the control group (2.9841 ng/ml). The mean fold change of miR-221 was significantly upregulated about six more times among HCV-exposed patients (mean = 6.3545) compared to the control group (mean = 1.1864). 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引用次数: 0

摘要

背景:丙型肝炎病毒(HCV)能够通过刺激细胞微小RNA(miRNA)的合成来改变细胞信使RNA的转录和翻译,从而损害免疫反应并促进病毒繁殖。抗HCV免疫反应中最重要的成员之一是核因子κB(NF-κB),它受到细胞miRNA的调节。目的:我们旨在研究HCV暴露个体血清NF-κB水平与循环miRNA-221(miR-221)倍数变化的相关性。材料和方法:采用酶联免疫吸附法测定88例样本(22例持续性丙型肝炎病毒感染者、22例自发性丙型肝炎病毒清除者、22名直接作用抗病毒药物治疗者和22名未感染的明显健康献血者作为对照)的血清NF-κB水平。逆转录聚合酶链式反应用于定量循环miR-221的表达倍数。结果:与对照组(2.9841 ng/ml)相比,暴露于HCV的患者(2.0058 ng/ml)在P<0.000时NF-κB的平均水平显著降低。与对照组(平均值=1.1864)相比,暴露于HCV的患者中miR-221的平均倍数变化显著上调了约6倍(平均值=6.3545)。此外,持续性HCV感染患者的miR-221倍数变化的平均±标准差显著高于DAA治疗后治愈的患者(P=0.048),血清NF-κB水平与miR-221折叠水平呈弱负相关(r=-0.246,P=0.021)。结论:HCV感染破坏了NF-κB的激活,导致miR-221的失调,这种失调在病毒清除后很长一段时间仍存在。因此,HCV暴露患者血清NF-κB和miR-221的定量可作为长期随访中的无创预后标志物。此外,miRNA图谱分析可以帮助区分暴露于HCV的健康个体。
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Correlation of NF-kB serum level with the expression pattern of microrna-221 in a sample of hcv-exposed Iraqi patients
Background: Hepatitis C virus (HCV) has the ability to change cellular messenger RNA transcription and translation by stimulating the synthesis of cellular microRNAs (miRNAs) that impair immune response and facilitate viral reproduction. One of the most important members of the immune response against HCV is nuclear factor-kappa B (NF-κB), which is regulated by cellular miRNAs. Aims: we aimed to investigate the correlation of NF-κB serum level with circulatory miRNA-221 (miR-221) fold change in HCV-exposed individuals. Materials and Methods: Serum level of NF-κB in 88 samples (22 patients with persistent HCV infection, 22 individuals with spontaneous HCV virus clearance, 22 individuals treated with direct-acting antivirals (DAAs) drugs, and 22 uninfected apparently healthy blood donors as control) was measured by enzyme-linked immunosorbent assay. Reverse transcriptase–polymerase chain reaction was used to quantify the expression fold of circulatory miR-221. Results: The results showed that there was a significant decrease in the mean level of NF-κB at P < 0.000 among HCV-exposed patients (2.0058 ng/ml) as compared to the control group (2.9841 ng/ml). The mean fold change of miR-221 was significantly upregulated about six more times among HCV-exposed patients (mean = 6.3545) compared to the control group (mean = 1.1864). Furthermore, the mean ± standard deviation of miR-221 fold change in patients with persistent HCV infection was significantly higher compared to patients cured after DAA therapy (P = 0.048), there was a weak negative correlation (r = −0.246, P = 0.021) between NF-κB serum level and miR-221 folding level. Conclusion: HCV infection disrupts NF-κB activation, resulting in dysregulation of miR-221 that persists long after the virus has been cleared. Thus, quantification of serum NF-κB and miR-221in HCV-exposed patients could be used as noninvasive prognostic marker during long-term follow-up. Furthermore, a miRNAs profile analysis can help distinguish HCV-exposed from healthy individuals.
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