首页> 外文期刊>The Journal of Experomental Medicine >Age at First Viral Infection Determines the Pattern of T Cell–mediated Disease during Reinfection in Adulthood
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Age at First Viral Infection Determines the Pattern of T Cell–mediated Disease during Reinfection in Adulthood

机译:初次病毒感染的年龄决定了成年期再感染期间T细胞介导的疾病的模式

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Infants experiencing severe respiratory syncytial virus (RSV) bronchiolitis have an increased frequency of wheeze and asthma in later childhood. Since most severe RSV infections occur between the 8th and 24th postnatal week, we examined whether age at first infection determines the balance of cytokine production and lung pathology during subsequent rechallenge. Primary RSV infection in newborn mice followed the same viral kinetics as in adults but was associated with reduced and delayed IFN-γ responses. To study rechallenge, mice were infected at 1 day or 1, 4, or 8 weeks of age and reinfected at 12 weeks. Neonatal priming produced more severe weight loss and increased inflammatory cell recruitment (including T helper 2 cells and eosinophils) during reinfection, whereas delayed priming led to enhanced interferon γ production and less severe disease during reinfection. These results show the crucial importance of age at first infection in determining the outcome of reinfection and suggest that the environment of the neonatal lung is a major determinant of cytokine production and disease patterns in later life. Thus, simply delaying RSV infection beyond infancy might reduce subsequent respiratory morbidity in later childhood.
机译:患有严重呼吸道合胞病毒(RSV)毛细支气管炎的婴儿在幼儿期出现喘息和哮喘的频率增加。由于最严重的RSV感染发生在产后第8周到第24周之间,因此我们检查了初次感染的年龄是否决定了随后的再攻击期间细胞因子产生和肺部病理的平衡。新生小鼠的原发性RSV感染遵循与成年相同的病毒动力学,但与减少和延迟的IFN-γ反应有关。为了研究挑战性,小鼠在1天或1、4、8周龄时感染,并在12周时再次感染。新生儿引发在重感染期间会导致更严重的体重减轻并增加炎症细胞募集(包括T辅助2细胞和嗜酸性粒细胞),而延迟引发则导致干扰素γ产生增加,并且在重新感染期间病情较轻。这些结果表明,初次感染时的年龄对于确定再感染的结果至关重要,并表明新生儿肺部环境是以后生命中细胞因子产生和疾病模式的主要决定因素。因此,仅将RSV感染推迟到婴儿期以后,就可以减少后来儿童的呼吸道发病率。

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