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Reduced PRF1 enhancer methylation in children with a history of severe RSV bronchiolitis in infancy: an association study

机译:婴儿严重RSV毛细支气管炎病史儿童PRF1增强子甲基化水平降低:一项关联研究

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Background Acute lower respiratory tract infection is the commonest disease affecting children under five worldwide. Respiratory syncytial virus (RSV) is among the most common causative pathogens. Epidemiological data suggest an association between severe viral respiratory infections in infancy and increased incidence of childhood wheeze and asthma. DNA methylation is involved in immune cell differentiation and identity. It provides an avenue for environmental influences on the genome and therefore has potential as a marker for sustained effects of infectious insults. In this study we investigated the association between DNA methylation patterns in the perforin gene ( PRF1 ) in childhood and a history of hospitalisation for severe RSV disease in the first two years of life. Methods In this retrospective study, we explored patterns of whole blood DNA methylation at a methylation sensitive region of the proximal PRF1 enhancer in a group of children with a record of hospitalisation for severe RSV disease during infancy ( n =?43) compared to healthy controls matched for age and sex with no similar hospitalisation history, no allergy and no persistent wheeze ( n =?43). Univariate and bivariate conditional logistic regression analyses were conducted to test the association between PRF1 enhancer methylation and record of hospitalisation for RSV disease. Results Children with a record of hospitalisation for severe RSV bronchiolitis demonstrated markedly lower levels of DNA methylation at two cytosine-phosphate-guanine dinucleotide (CpG) loci of the PRF1 proximal enhancer, corresponding to a signal transducer and activator of transcription 5 (STAT5) responsive element, compared to controls, adjusted odds ratios of 0.82 (95% confidence interval [CI] 0.71, 0.94) and 0.73 (95% CI 0.58, 0.92) for each 1% increase in DNA methylation. Smoking in the household showed a significant influence on DNA methylation at the assayed positions. Conclusions Our findings support an association between childhood DNA methylation patterns in PRF1 and a record of severe RSV infection in infancy. Longitudinal studies are required to establish the utility of PRF1 methylation as a marker of severe RSV disease.
机译:背景技术急性下呼吸道感染是影响全球五岁以下儿童的最常见疾病。呼吸道合胞病毒(RSV)是最常见的致病菌。流行病学数据表明,婴儿期严重的病毒性呼吸道感染与儿童喘息和哮喘的发生率增加之间存在关联。 DNA甲基化参与免疫细胞的分化和鉴定。它为环境对基因组的影响提供了途径,因此有潜力作为感染性侵害持续影响的标志。在这项研究中,我们调查了儿童穿孔素基因(PRF1)中的DNA甲基化模式与出生后头两年严重RSV疾病住院史的关系。方法在这项回顾性研究中,我们探索了一组在婴儿期有严重RSV疾病住院记录的儿童(n = 43)与健康对照组相比,在近端PRF1增强子甲基化敏感区域的全血DNA甲基化模式。年龄和性别相匹配,没有相似的住院病史,没有过敏,也没有持续性喘息(n =?43)。进行单因素和双因素条件logistic回归分析,以检验PRF1增强子甲基化与RSV疾病住院记录之间的关联。结果有严重RSV毛细支气管炎住院记录的儿童在PRF1近端增强子的两个胞嘧啶-磷酸-鸟嘌呤二核苷酸(CpG)位点表现出明显较低的DNA甲基化水平,对应于信号转导子和转录激活子5(STAT5)响应与对照组相比,DNA甲基化水平每提高1%,调整后的优势比分别为0.82(95%置信区间[CI] 0.71,0.94)和0.73(95%CI 0.58,0.92)。家庭中的吸烟对检测位置的DNA甲基化有重要影响。结论我们的发现支持PRF1中儿童期DNA甲基化模式与婴儿期严重RSV感染的记录之间的关联。需要进行纵向研究以建立PRF1甲基化作为严重RSV疾病标记的效用。

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