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Biochemical and molecular study on serum miRNA-16a and miRNA- 451 as neonatal sepsis biomarkers

机译:血清miRNA-16a和miRNA-451的生化和分子研究作为新生儿败血症生物标志物

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BackgroundSepsis is the serious cause of fatality in the unit of medical-intensive care (ICU). Non-coding RNA transcripts are microRNA that control gene expression by repressing translation or degrading mRNA. There are several reports discussing the concept of using miRNAs as sepsis a biomarkers by profiling miRNA dysregulation in sepsis patients' blood samples.ObjectivesThe research was aimed at exploring the clinical utility of miRNA-16a and miRNA- 451 for diagnosis of neonatal sepsis.Subjectsand methods: This research was conducted on 50 full term neonates, 25 neonates with suspected or proven sepsis and 25 clinically healthy sex and age matched neonates with no evidence of sepsis. All newborns have been exposed to clinical review, history taking and laboratory investigations including total & differential count of blood cells, C-reactive protein, blood culture. Serum miRNA-16a and miRNA-451 levels have been assessed using Real Time polymerase chain reaction (Real Time PCR) technique.ResultsNeonates with sepsis had considerably higher levels of miRNA-16a and miRNA- 451 than the healthy neonates (p?≤?0.001). Receiver operating curve (ROC) showed that serum miRNA-16a was superior to miRNA-451 for diagnosis of sepsis with neonatal origin; it had sensitivity and specificity of 88% and 98% versus 64% and 61% respectively. Cut off point for miRNA-16a to diagnose neonatal sepsis was above or equal 3.16. Also, cut off point for miRNA-451 was above or equal 1.26. miRNA-16 a and miRNA 451 expression was significantly correlated with respiratory rate, WBCs, and CRP.ConclusionBoth miRNA ?16a and miRNA-451 are detected in higher levels in newborn with sepsis compared to controls. MiRNA- 16a could be considered as promising biomarkers for diagnosis of neonatal sepsis.
机译:BackgroundseSES是医疗密集护理单位(ICU)的严重死亡原因。非编码RNA转录物是通过抑制平移或降解的mRNA来控制基因表达的microRNA。有几个报告讨论使用miRNA作为脓毒症的概念,通过在脓毒症患者的血液样本中分析miRNA失调的生物标志物。目前研究旨在探索miRNA-16a和miRNA-451的临床效用,用于诊断新生儿脓血的诊断:这项研究是在50个全年新生儿中进行的,25名新生儿,疑似或经过疑虑的脓毒症和25个临床健康的性和年龄匹配的新生儿,没有败血症的证据。所有新生儿都接触到临床审查,历史和实验室调查,包括总&血细胞,C反应蛋白,血液培养的差异计数。已经使用实时聚合酶链反应(实时PCR)技术评估血清miRNA-16a和miRNA-451水平。与败血症的细胞酸糖酸盐比健康的新生儿的miRNA-16a和miRNA-451水平相当高(P?≤≤0.001 )。接收器操作曲线(ROC)显示血清MiRNA-16a优于miRNA-451,用于诊断新生儿的脓毒症;它的敏感性和特异性分别为88%和98%,分别为64%和61%。切断miRNA-16a以诊断新生儿败血症的点高于或等于3.16。此外,MiRNA-451的切断点高于或等于1.26。 miRNA-16a和miRNA 451表达与呼吸速率,WBC和CRP显着相关。与对照相比,在新生儿中,在新生儿中较高水平检测到miRNAα16a和miRNA-451。 miRNA-16a可以被认为是诊断新生儿败血症的有前途的生物标志物。

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