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Systemic T-helper and T-regulatory cell type cytokine responses in rhinovirus vs. respiratory syncytial virus induced early wheezing: an observational study

机译:鼻病毒与呼吸道合胞病毒引起的早期喘息的全身性T辅助和T调节细胞型细胞因子反应:一项观察性研究

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BackgroundRhinovirus (RV) associated early wheezing has been recognized as an independent risk factor for asthma. The risk is more important than that associated with respiratory syncytial virus (RSV) disease. No comparative data are available on the immune responses of these diseases.ObjectiveTo compare T-helper1 (Th1), Th2 and T-regulatory (Treg) cell type cytokine responses between RV and RSV induced early wheezing.MethodsSystemic Th1-type (interferon [IFN] -gamma, interleukin [IL] -2, IL-12), Th2-type (IL-4, IL-5, IL-13) and Treg-type (IL-10) cytokine responses were studied from acute and convalescence phase serum samples of sole RV (n = 23) and RSV affected hospitalized wheezing children (n = 27). The pre-defined inclusion criteria were age of 3-35 months and first or second wheezing episode. Analysis was adjusted for baseline differences. Asymptomatic children with comparable demographics (n = 11) served as controls for RV-group.ResultsRV-group was older and had more atopic characteristics than RSV-group. At acute phase, RV-group had higher (fold change) IL-13 (39-fold), IL-12 (7.5-fold), IFN-gamma (6.0-fold) and IL-5 (2.8-fold) concentrations than RSV-group and higher IFN-gamma (27-fold), IL-2 (8.9-fold), IL-5 (5.6-fold) and IL-10 (2.6-fold) than the controls. 2-3 weeks later, RV-group had higher IFN-gamma (>100-fold), IL-13 (33-fold) and IL-10 (6.5-fold) concentrations than RSV-group and higher IFN-gamma (15-fold) and IL-2 (9.4-fold) than the controls. IL-10 levels were higher in acute phase compared to convalescence phase in both infections (p < 0.05 for all).ConclusionOur results support a hypothesis that RV is likely to trigger wheezing mainly in children with a predisposition. IL-10 may have important regulatory function in acute viral wheeze.
机译:背景鼻病毒(RV)相关的早期喘息已被认为是哮喘的独立危险因素。该风险比与呼吸道合胞病毒(RSV)疾病相关的风险更为重要。目前尚无关于这些疾病的免疫反应的比较数据。目的比较RV和RSV诱导的早期喘息中T-helper1(Th1),Th2和T调节(Treg)细胞型细胞因子的反应。从急性期和恢复期研究了]-γ,白介素[IL] -2,IL-12,Th2型(IL-4,IL-5,IL-13)和Treg型(IL-10)的细胞因子反应。唯一的RV(n = 23)和RSV感染的住院喘息儿童(n = 27)的血清样本。预先确定的入选标准为3-35个月大以及第一次或第二次喘息发作。调整分析的基线差异。 RV组的对照组为无症状儿童(n = 11)。结果RV组比RSV组年龄大,特应性特征也好。在急性期,RV组的IL-13(39倍),IL-12(7.5倍),IFN-γ(6.0倍)和IL-5(2.8倍)浓度较高(变化)。与对照组相比,RSV组和更高的IFN-γ(27倍),IL-2(8.9倍),IL-5(5.6倍)和IL-10(2.6倍)。 2-3周后,RV组的IFN-γ浓度(> 100倍),IL-13(33倍)和IL-10(6.5倍)的浓度高于RSV组和IFN-γ(15倍)和IL-2(9.4倍)。在两种感染中,急性期的IL-10水平均高于恢复期(所有情况均p <0.05)。结论我们的结果支持以下假设:RV可能主要在易感儿童中引发喘息。 IL-10在急性病毒性喘息中可能具有重要的调节功能。

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