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2018 年英国肠道病毒 D68 疫情由亚群 B3 和 D1 引起,分别主要发生在儿童和成人中,两个亚群均表现出广泛的遗传多样性。

Enterovirus D68 epidemic, UK, 2018, was caused by subclades B3 and D1, predominantly in children and adults, respectively, with both subclades exhibiting extensive genetic diversity.

机构信息

Clinical Microbiology, Nottingham University Hospitals NHS Trust, Nottingham, UK.

School of Life Sciences, University of Nottingham, Nottingham, UK.

出版信息

Microb Genom. 2022 May;8(5). doi: 10.1099/mgen.0.000825.

DOI:10.1099/mgen.0.000825
PMID:35532121
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9465064/
Abstract

Enterovirus D68 (EV-D68) has recently been identified in biennial epidemics coinciding with diagnoses of non-polio acute flaccid paralysis/myelitis (AFP/AFM). We investigated the prevalence, genetic relatedness and associated clinical features of EV-D68 in 193 EV-positive samples from 193 patients in late 2018, UK. EV-D68 was detected in 83 (58 %) of 143 confirmed EV-positive samples. Sequencing and phylogenetic analysis revealed extensive genetic diversity, split between subclades B3 (=50) and D1 (=33), suggesting epidemiologically unrelated infections. B3 predominated in children and younger adults, and D1 in older adults and the elderly (=0.0009). Clinical presentation indicated causation or exacerbation of respiratory distress in 91.4 % of EV-D68-positive individuals, principally cough (75.3 %), shortness of breath (56.8 %), coryza (48.1 %), wheeze (46.9 %), supplemental oxygen required (46.9 %) and fever (38.9 %). Two cases of AFM were observed, one with EV-D68 detectable in the cerebrospinal fluid, but otherwise neurological symptoms were rarely reported (=4). Both AFM cases and all additional instances of intensive care unit (ICU) admission (=5) were seen in patients infected with EV-D68 subclade B3. However, due to the infrequency of severe infection in our cohort, statistical significance could not be assessed.

摘要

肠道病毒 D68(EV-D68)最近在两年一次的流行中被发现,与非脊髓灰质炎急性弛缓性麻痹/脊髓灰质炎(AFP/AFM)的诊断相一致。我们调查了 2018 年底英国 193 名 EV 阳性患者的 193 份样本中 EV-D68 的流行率、遗传相关性和相关临床特征。在 143 份经证实的 EV 阳性样本中,有 83 份(58%)检测到 EV-D68。测序和系统发育分析显示存在广泛的遗传多样性,分为子群 B3(=50)和 D1(=33),提示存在流行病学上无关的感染。B3 主要在儿童和年轻成年人中流行,而 D1 在老年人和老年人中流行(=0.0009)。临床表现表明,91.4%的 EV-D68 阳性个体存在呼吸窘迫的原因或加重,主要表现为咳嗽(75.3%)、呼吸急促(56.8%)、鼻塞(48.1%)、哮鸣音(46.9%)、需要补充氧气(46.9%)和发热(38.9%)。观察到 2 例 AFM,1 例脑脊液中可检测到 EV-D68,但其他神经系统症状很少报告(=4)。在感染 EV-D68 子群 B3 的患者中,均观察到 AFM 病例和所有其他 ICU 入院病例(=5)。然而,由于我们的队列中严重感染的频率较低,因此无法评估统计学意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7c19/9465064/4b2368568662/mgen-8-825-g006.jpg
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https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7c19/9465064/8121aab8d4ea/mgen-8-825-g002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7c19/9465064/d379448ba92f/mgen-8-825-g003.jpg
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