Jaligama Sridhar, Saravia Jordy, You Dahui, Yadav Nikki, Lee Greg I, Shrestha Bishwas, Cormier Stephania A
Children's Foundation Research Institute, Le Bonheur Children's Hospital, 50 N Dunlap Street, Memphis, TN, 38103, USA.
Department of Pediatrics, The University of Tennessee Health Science Center, Translational Research Science Bldg. 71S Manassas, Suite 430J, Memphis, TN, 38103, USA.
Respir Res. 2017 Jan 13;18(1):15. doi: 10.1186/s12931-016-0487-4.
Exposure to elevated levels of particulate matter (PM) is associated with increased risk of morbidity and mortality due to respiratory tract viral infections in infants. Recent identification of environmentally persistent free radicals (EPFRs) in the PM from a variety of combustion sources suggests its role in the enhancement of disease severity of lower respiratory tract infections (LRTI). Our previous studies demonstrated that acute exposure to EPFRs induces pulmonary immunosuppression allowing for enhanced influenza disease severity. Here, we determine the mechanism of EPFR-induced immunosuppression and its impact on the immune response towards influenza infection.
Neonatal mice (3 days old) were acutely exposed to DCB (combustion derived PM with chemisorbed EPFR) for seven consecutive days. Four days post-exposure (dpe), mice were infected with influenza virus. Pulmonary T cell phenotypes including regulatory T cells (Tregs) were analyzed by flow cytometry. The role of IL10 in EPFR-induced exacerbation of influenza disease severity was determined by administering recombinant IL10 (rIL10) to wild type mice or by using IL10 deficient (IL10) neonatal mice. Mice were assessed for morbidity by measuring percent weight change and pulmonary viral load.
Neonatal mice exposed to EPFRs had a significant increase in pulmonary Tregs and the immunosuppressive cytokine IL10 following influenza infection, which coincided with decreased protective T cell responses to influenza infection at 6 dpi. Depletion of Tregs in EPFR-exposed neonatal mice resulted in increased protective, adaptive T cell responses, whereas adoptive transfer of Tregs from EPFR-exposed neonates to air-exposed neonatal mice suppressed adaptive T cell responses towards influenza infection. Further, treatment with rIL10 could recapitulate EPFR-induced exacerbation of morbidity and pulmonary viral load compared to air exposed and influenza infected mice, whereas, EPFR-exposed IL10 neonates exhibited significant reductions in morbidity, pulmonary viral load and adaptive T cell responses following influenza infection.
Neonatal exposure to EPFRs induced Tregs and IL10 resulting in suppressed adaptive T cell responses and enhanced influenza disease severity in neonatal mice. Depletion of Tregs increased adaptive T cell responses and deficiency of IL10 reduced morbidity and conferred enhanced protection against influenza virus.
暴露于高水平的颗粒物(PM)与婴儿因呼吸道病毒感染导致的发病和死亡风险增加有关。最近在各种燃烧源的PM中发现了环境持久性自由基(EPFRs),这表明其在加重下呼吸道感染(LRTI)疾病严重程度方面的作用。我们之前的研究表明,急性暴露于EPFRs会诱导肺部免疫抑制,从而加重流感疾病的严重程度。在此,我们确定EPFR诱导免疫抑制的机制及其对流感感染免疫反应的影响。
新生小鼠(3日龄)连续7天急性暴露于DCB(含有化学吸附EPFR的燃烧源PM)。暴露后4天(dpe),小鼠感染流感病毒。通过流式细胞术分析包括调节性T细胞(Tregs)在内的肺T细胞表型。通过向野生型小鼠施用重组IL10(rIL10)或使用IL10缺陷型(IL10 -/-)新生小鼠来确定IL10在EPFR诱导的流感疾病严重程度加重中的作用。通过测量体重变化百分比和肺病毒载量来评估小鼠的发病率。
暴露于EPFRs的新生小鼠在感染流感后肺Tregs和免疫抑制细胞因子IL10显著增加,这与6 dpi时对流感感染的保护性T细胞反应降低相一致。在暴露于EPFRs的新生小鼠中耗尽Tregs导致保护性适应性T细胞反应增加,而将暴露于EPFRs的新生小鼠的Tregs过继转移到暴露于空气的新生小鼠中则抑制了对流感感染的适应性T细胞反应。此外,与暴露于空气和感染流感的小鼠相比,用rIL10治疗可重现EPFR诱导的发病率和肺病毒载量加重,而暴露于EPFRs的IL10 -/-新生小鼠在感染流感后发病率、肺病毒载量和适应性T细胞反应显著降低。
新生小鼠暴露于EPFRs会诱导Tregs和IL10,导致适应性T细胞反应受到抑制,并加重新生小鼠的流感疾病严重程度。耗尽Tregs会增加适应性T细胞反应,而IL10缺陷会降低发病率并增强对流感病毒的保护作用。
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