婴儿临床呼吸道合胞病毒疾病严重程度差异的病毒特异性因素

Clinical microbiology (Los Angeles, Calif.) Pub Date : 2015-06-01 Epub Date: 2015-06-29 DOI:10.4172/2327-5073.1000206

Tonya M Thompson, Philippa L Roddam, Lisa M Harrison, Jody A Aitken, John P DeVincenzo

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引用次数: 22

摘要

背景:在以前健康的婴儿中，呼吸道合胞病毒(RSV)疾病的严重程度范围很广。宿主因素已被充分证明有助于疾病严重程度的差异。然而，由病毒本身固有的因素造成疾病严重程度差异的可能性很少得到研究。方法:在保持宿主因素不变的情况下，从不同RSV疾病严重程度的婴儿中前瞻性采集低传代RSV分离株，在体外进行评估，以评估分离株是否在人肺上皮细胞系中诱导表型不同的细胞因子/趋化因子浓度。将67株来自健康婴儿的RSV分离株(38例因急性RSV感染住院治疗(重症)，29例从未住院治疗(轻症))接种到A549肺上皮细胞中，在精确控制的低多重感染下模拟自然感染。在48小时、60小时和72小时对培养物进行评估，以评估细胞因子/趋化因子诱导的曲线下面积(AUC)。结果:感染重症婴儿分离物的细胞在所有测试点产生更高的所有细胞因子/趋化因子(IL-1α， IL-6, IL-8和RANTES)的平均浓度。重症患儿RSV分离株在感染培养物中AUCIL-8和AUCRANTES的分泌明显高于轻症患儿(p=0.028和p=0.019)。在这些重症分离的婴儿中，IL-8和RANTES浓度在48小时时高出4倍。此外，在所有时间点对38株分离物的病毒数量进行了评估。RSV浓度与各时间点IL-8和RANTES均显著相关。细胞因子/趋化因子浓度和RSV浓度均与RSV亚组无关。讨论:婴儿RSV疾病严重程度的差异可能部分归因于内在的病毒株特异性特征。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Viral Specific Factors Contribute to Clinical Respiratory Syncytial Virus Disease Severity Differences in Infants.

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Viral Specific Factors Contribute to Clinical Respiratory Syncytial Virus Disease Severity Differences in Infants.

Background: There is a wide range of severity of respiratory syncytial viral (RSV) disease in previously healthy infants. Host factors have been well demonstrated to contribute to disease severity differences. However the possibility of disease severity differences being produced by factors intrinsic to the virus itself has rarely been studied.

Methods: Low-passage isolates of RSV collected prospectively from infants with different degrees of RSV disease severity were evaluated in vitro, holding host factors constant, so as to assess whether isolates induced phenotypically different cytokine/chemokine concentrations in a human lung epithelial cell line. Sixty-seven RSV isolates from previously healthy infants (38 hospitalized for acute RSV infection (severe disease) and 29 never requiring hospitalization (mild disease)) were inoculated into A549, lung epithelial cells at precisely controlled, low multiplicity of infection to mimic natural infection. Cultures were evaluated at 48 hours, 60 hours, and 72 hours to evaluate area under the curve (AUC) cytokine/chemokine induction.

Results: Cells infected with isolates from severely ill infants produced higher mean concentrations of all cytokine/chemokines tested (IL-1α, IL-6, IL-8 and RANTES) at all-time points tested. RSV isolates collected from infants with severe disease induced significantly higher AUCIL-8 and AUCRANTES secretion in infected cultures than mild disease isolates (p=0.028 and p=0.019 respectively). IL-8 and RANTES concentrations were 4 times higher at 48 hours for these severely ill infant isolates. Additionally, 38 isolates were evaluated at all-time points for quantity of virus. RSV concentration significantly correlated with both IL-8 and RANTES at all-time points. Neither cytokine/chemokine concentrations nor RSV concentrations were associated with RSV subgroup.

Discussion: Infants' RSV disease severity differences may be due in part to intrinsic viral strain-specific characteristics.

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Clinical microbiology (Los Angeles, Calif.)

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