Pelullo Maria, Savi Daniela, Quattrucci Serena, Cimino Giuseppe, Pizzuti Antonio, Screpanti Isabella, Talora Claudio, Cialfi Samantha
Center for Life Nano Science@Sapienza, Istituto Italiano di Tecnologia, I-00161 Rome, Italy.
Department of Public Health and Infectious Diseases, Sapienza University of Rome, I-00161 Rome, Italy.
Exp Ther Med. 2021 Jun;21(6):585. doi: 10.3892/etm.2021.10017. Epub 2021 Apr 2.
In the physiopathology of cystic fibrosis (CF), oxidative stress implications are recognized and widely accepted. The cystic fibrosis transmembrane conductance regulator (CFTR) defects disrupt the intracellular redox balance causing CF pathological hallmarks. Therefore, oxidative stress together with aberrant expression levels of detoxification genes and microRNAs (miRNAs/miRs) may be associated with clinical outcome. Using total RNA extracted from epithelial nasal cells, the present study analyzed the expression levels of oxidative stress genes and one miRNA using quantitative PCR in a representative number of patients with CF compared with in healthy individuals. The present pilot study revealed the existence of an association among CFTR, genes involved in the oxidative stress response and miR-125b. The observed downregulation of CFTR gene expression was accompanied by increased expression levels of Nuclear factor erythroid derived-2 like2 and its targets NAD(P)H:Quinone Oxidoreductase and glutathione S-transferase 1. Moreover, the expression levels of heme oxygenase-1 (HO-1) and miR-125b were positively correlated with a forced expiratory volume in 1 sec (FEV1) >60% in patients with CF with chronic lung infection (r=0.74; P<0.001 and r=0.57; P<0.001, respectively). The present study revealed the activation of an inducible, but not fully functional, oxidative stress response to protect airway cells against reactive oxygen species-dependent injury in CF disease. Additionally, the correlations of HO-1 and miR-125b expression with an improved FEV1 value suggested that these factors may synergistically protect the airway cells from oxidative stress damage, inflammation and apoptosis. Furthermore, HO-1 and miR-125b may be used as prognostic markers explaining the wide CF phenotypic variability as an additional control level over the CFTR gene mutations.
在囊性纤维化(CF)的生理病理学中,氧化应激的影响已得到认可并被广泛接受。囊性纤维化跨膜传导调节因子(CFTR)缺陷会破坏细胞内氧化还原平衡,导致CF的病理特征。因此,氧化应激以及解毒基因和微小RNA(miRNA/miR)的异常表达水平可能与临床结果相关。本研究使用从鼻上皮细胞中提取的总RNA,通过定量PCR分析了具有代表性数量的CF患者与健康个体相比氧化应激基因和一种miRNA的表达水平。本初步研究揭示了CFTR、参与氧化应激反应的基因和miR-125b之间存在关联。观察到的CFTR基因表达下调伴随着核因子红细胞衍生2样2及其靶标NAD(P)H:醌氧化还原酶和谷胱甘肽S-转移酶1表达水平的增加。此外,在患有慢性肺部感染的CF患者中,血红素加氧酶-1(HO-1)和miR-125b的表达水平与一秒用力呼气量(FEV1)>60%呈正相关(分别为r=0.74;P<0.001和r=0.57;P<0.001)。本研究揭示了一种诱导性但未完全发挥功能的氧化应激反应的激活,以保护气道细胞免受CF疾病中活性氧依赖性损伤。此外,HO-1和miR-125b表达与改善的FEV1值之间的相关性表明,这些因素可能协同保护气道细胞免受氧化应激损伤、炎症和凋亡。此外,HO-1和miR-125b可用作预后标志物,作为CFTR基因突变之外的额外控制水平来解释CF广泛的表型变异性。