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分子多样性和肠病毒 D68 的两年循环:法国里昂 2010 至 2016 年的系统筛查研究。

Molecular diversity and biennial circulation of enterovirus D68: a systematic screening study in Lyon, France, 2010 to 2016.

机构信息

Centre National de Référence des Enterovirus et Parechovirus, Laboratoire de Virologie, Institut des Agents Infectieux, HCL, Hôpital de la Croix-Rousse, Lyon, France.

European Public Health Microbiology Training Programme (EUPHEM), European Centre for Disease Prevention and Control, Stockholm, Sweden.

出版信息

Euro Surveill. 2018 Sep;23(37). doi: 10.2807/1560-7917.ES.2018.23.37.1700711.

Abstract

BackgroundUnderstanding enterovirus D68 (EV-D68) circulation patterns as well as risk factors for severe respiratory and neurological illness is important for developing preventive strategies. : Between 2010 and 2016, 11,132 respiratory specimens from hospitalised patients in Lyon, France, were screened for EV-D68 by PCR. Phylogenetic relationships of the viral-protein-1 sequences were reconstructed using maximum-likelihood and Bayesian-Markov-Chain-Monte-Carlo approaches. Overall, 171 infections with a biennial pattern were detected, including seven, one, 55, none, 42, one and 65 cases annually during 2010-16. Children (< 16 years-old; n = 150) were mostly affected and 71% (n = 121) of the total patients were under 5 years-old. In 146 patients with medical reviews, 73% (n = 107) presented with acute respiratory distress. Among paediatric patients with medical reviews (n = 133), 55% (n=73) had an asthma/wheezing history, while among adults (n = 13), 11 had underlying diseases. In total, 45 patients had severe infections and 28 patients needed intensive care unit stays. No acute flaccid myelitis (AFM) was detected. We found genotypes A, B1, B2 B3 and D circulating, and no associations between these and clinical presentations. During the study, new genotypes continuously emerged, being replaced over time. We estimated that ancestors of currently circulating genotypes emerged in the late-1990s to 2010. Rises of the EV-D68 effective population size in Lyon coincided with infection upsurges. Phylogenetic analyses showed ongoing diversification of EV-D68 worldwide, coinciding with more infections in recent years and increases of reported AFM paediatric cases. Reinforcement of diagnostic capacities and clinical-based surveillance of EV-D68 infections is needed in Europe to assess the EV-D68 burden.

摘要

背景

了解肠道病毒 D68(EV-D68)的循环模式以及导致严重呼吸道和神经系统疾病的危险因素对于制定预防策略非常重要。方法:在 2010 年至 2016 年间,对法国里昂住院患者的 11132 份呼吸道标本进行了 EV-D68 的 PCR 检测。采用最大似然法和贝叶斯-马尔可夫链-蒙特卡罗法重建病毒蛋白-1 序列的系统进化关系。结果:共检测到 171 例呈两年周期性的感染,包括 2010-2016 年每年 7、1、55、0、42、1 和 65 例。儿童(<16 岁;n=150)受影响最大,146 例有医疗记录的患者中 71%(n=121)年龄小于 5 岁。在 146 例有医疗记录的患者中,73%(n=107)出现急性呼吸窘迫。在有医疗记录的儿科患者(n=133)中,55%(n=73)有哮喘/喘息史,而在成年人(n=13)中,11 人有潜在疾病。共有 45 例患者出现严重感染,28 例患者需要入住重症监护病房。未发现急性弛缓性脊髓炎(AFM)。我们发现了 A、B1、B2、B3 和 D 基因型在循环,并且这些与临床表型之间没有关联。在研究期间,新的基因型不断出现,并随着时间的推移被取代。我们估计目前循环基因型的祖先出现在 20 世纪 90 年代末至 2010 年。里昂 EV-D68 有效种群数量的增加与感染的增加相吻合。系统进化分析显示,全球范围内 EV-D68 正在不断多样化,这与近年来感染病例的增加和报告的 AFM 儿科病例的增加相一致。结论:欧洲需要加强对 EV-D68 感染的诊断能力和基于临床的监测,以评估 EV-D68 的负担。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d66b/6144471/dad0173b0663/1700711-f1.jpg

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