Genetics Unit, Department of Histology and Cell Biology, Faculty of Medicine, Suez Canal University, Ismailia, P.O. 41522, Egypt.
Pulmonologist, Ministry of Health, Cairo, Egypt.
Respir Res. 2017 Sep 8;18(1):169. doi: 10.1186/s12931-017-0648-0.
Small non-coding RNAs (microRNAs) have been evolved to master numerous cellular processes. Genetic variants within microRNA seed region might influence microRNA biogenesis and function. The study aimed at determining the role of microRNA-499 (MIR-499) gene family polymorphism as a marker for susceptibility and progression of bronchial asthma and to analyze the structural and functional impact of rs3746444 within the seed region.
Genotyping for 192 participants (96 patients and 96 controls) in the discovery phase and 319 subjects (115 patients and 204 controls) in the replication phase was performed via Real Time-Polymerase Chain Reaction technology. Patients underwent the methacholine challenge test and biochemical analysis. Gene structural and functional analysis, target prediction, annotation clustering, and pathway enrichment analysis were executed. Predicted functional effect of rs37464443 SNP was analyzed.
miR-499 gene family is highly implicated in inflammation-related signaling pathways. Rs374644 (A > G) in MIR499A and MIR499B within the seed region could disrupt target genes and create new genes. The G variant was associated with high risk of developing asthma under all genetic association models (G versus A: OR = 3.27, 95% CI = 2.53-4.22; GG versus AA: OR = 9.52, 95% CI = 5.61-16.5; AG versus AA: OR = 2.13, 95% CI = 1.24-3.46; GG + AG versus AA: OR = 4.43, 95% CI = 2.88-6.82). GG genotype was associated with poor pre-bronchodilator FEV (p = 0.047) and the worst bronchodilator response after Salbutamol inhalation, represented in low peaked expiratory flow rate (p = 0.035).
miR-499 rs3746444 (A > G) polymorphism was associated with asthma susceptibility and bronchodilator response in Egyptian children and adolescents. Further functional analysis is warranted to develop more specific theranostic agents for selecting targeted therapy.
小非编码 RNA(microRNAs)已进化到能够掌控众多细胞过程。miRNA 种子区域内的遗传变异可能会影响 miRNA 的生物发生和功能。本研究旨在确定 microRNA-499(MIR-499)基因家族多态性作为支气管哮喘易感性和进展的标志物的作用,并分析种子区域内 rs3746444 对结构和功能的影响。
在发现阶段对 192 名参与者(96 名患者和 96 名对照)和复制阶段的 319 名受试者(115 名患者和 204 名对照)进行了 miR-499 基因家族多态性的基因分型,采用实时聚合酶链反应技术。患者接受了乙酰甲胆碱挑战试验和生化分析。进行了基因结构和功能分析、靶基因预测、注释聚类和通路富集分析。分析了 rs37464443 SNP 的预测功能效应。
miR-499 基因家族与炎症相关信号通路密切相关。种子区域内的 MIR499A 和 MIR499B 中的 rs374644(A>G)可能破坏靶基因并产生新基因。在所有遗传关联模型下,G 变体与哮喘发病风险增加相关(G 与 A:OR=3.27,95%CI=2.53-4.22;GG 与 AA:OR=9.52,95%CI=5.61-16.5;AG 与 AA:OR=2.13,95%CI=1.24-3.46;GG+AG 与 AA:OR=4.43,95%CI=2.88-6.82)。GG 基因型与预支气管扩张剂 FEV 不良相关(p=0.047),沙丁胺醇吸入后支气管扩张剂反应最差,表现为呼气高峰流量低(p=0.035)。
miR-499 rs3746444(A>G)多态性与埃及儿童和青少年的哮喘易感性和支气管扩张剂反应相关。需要进一步的功能分析来开发更特异的治疗诊断试剂,以选择靶向治疗。
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