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通过对雪貂眼部接种检测空气中的甲型流感病毒和 SARS-CoV-2 病毒的释放。

Detection of Airborne Influenza A and SARS-CoV-2 Virus Shedding following Ocular Inoculation of Ferrets.

机构信息

Influenza Division, Centers for Disease Control and Preventiongrid.416738.f, Atlanta, Georgia, USA.

出版信息

J Virol. 2022 Dec 21;96(24):e0140322. doi: 10.1128/jvi.01403-22. Epub 2022 Nov 30.

Abstract

Despite reports of confirmed human infection following ocular exposure with both influenza A virus (IAV) and SARS-CoV-2, the dynamics of virus spread throughout oculonasal tissues and the relative capacity of virus transmission following ocular inoculation remain poorly understood. Furthermore, the impact of exposure route on subsequent release of airborne viral particles into the air has not been examined previously. To assess this, ferrets were inoculated by the ocular route with A(H1N1)pdm09 and A(H7N9) IAVs and two SARS-CoV-2 (early pandemic Washington/1 and Delta variant) viruses. Virus replication was assessed in both respiratory and ocular specimens, and transmission was evaluated in direct contact or respiratory droplet settings. Viral RNA in aerosols shed by inoculated ferrets was quantified with a two-stage cyclone aerosol sampler (National Institute for Occupational Safety and Health [NIOSH]). All IAV and SARS-CoV-2 viruses mounted a productive and transmissible infection in ferrets following ocular inoculation, with peak viral titers and release of virus-laden aerosols from ferrets indistinguishable from those from ferrets inoculated by previously characterized intranasal inoculation methods. Viral RNA was detected in ferret conjunctival washes from all viruses examined, though infectious virus in this specimen was recovered only following IAV inoculation. Low-dose ocular-only aerosol exposure or inhalation aerosol exposure of ferrets to IAV similarly led to productive infection of ferrets and shedding of aerosolized virus. Viral evolution during infection was comparable between all inoculation routes examined. These data support that both IAV and SARS-CoV-2 can establish a high-titer mammalian infection following ocular exposure that is associated with rapid detection of virus-laden aerosols shed by inoculated animals. Documented human infection with influenza viruses and SARS-CoV-2 has been reported among individuals wearing respiratory protection in the absence of eye protection, highlighting the capacity of these respiratory tract-tropic viruses to exploit nonrespiratory routes of exposure to initiate productive infection. However, comprehensive evaluations of how ocular exposure may modulate virus pathogenicity and transmissibility in mammals relative to respiratory exposure are limited and have not investigated multiple virus families side by side. Using the ferret model, we show that ocular exposure with multiple strains of either coronaviruses or influenza A viruses leads to an infection that results in shedding of detectable aerosolized virus from inoculated animals, contributing toward onward transmission of both viruses to susceptible contacts. Collectively, these studies support that the ocular surface represents a susceptible mucosal surface that, if exposed to a sufficient quantity of either virus, permits establishment of an infection which is similarly transmissible as that following respiratory exposure.

摘要

尽管有报道称,在眼部接触流感病毒(IAV)和严重急性呼吸综合征冠状病毒 2 型(SARS-CoV-2)后,确实会发生人类感染,但病毒在眼鼻组织中的传播动力学以及眼部接种后病毒传播的相对能力仍知之甚少。此外,以前没有研究过暴露途径对随后空气中空气传播病毒颗粒释放的影响。为了评估这一点,我们通过眼部途径将 A(H1N1)pdm09 和 A(H7N9)IAV 以及两种 SARS-CoV-2(早期大流行的华盛顿/1 型和 Delta 变体)病毒接种到雪貂体内。在呼吸道和眼部标本中评估了病毒复制情况,并在直接接触或呼吸道飞沫环境中评估了传播情况。使用两级旋风气溶胶采样器(美国国家职业安全与健康研究所 [NIOSH])定量检测接种雪貂释放的气溶胶中的病毒 RNA。在眼部接种后,所有 IAV 和 SARS-CoV-2 病毒在雪貂体内均引发了具有传染性和可传播性的感染,病毒滴度峰值和携带病毒的气溶胶从雪貂体内释放与先前通过鼻腔接种方法接种的雪貂相同。从所有检查的病毒中均检测到雪貂结膜冲洗液中的病毒 RNA,但仅在接种 IAV 后才从该标本中回收具有传染性的病毒。低剂量的眼部仅气溶胶暴露或吸入气溶胶暴露于 IAV 的雪貂同样导致雪貂感染并释放气溶胶化病毒。在所有检查的接种途径中,病毒进化情况相似。这些数据支持 IAV 和 SARS-CoV-2 均可在眼部暴露后在哺乳动物中建立高滴度感染,这与接种动物释放携带病毒的气溶胶的快速检测有关。有记录的人类感染流感病毒和 SARS-CoV-2 已在未戴护目镜而仅戴呼吸防护装备的个体中报告,这突出表明这些呼吸道嗜性病毒能够利用非呼吸道暴露途径来引发有感染力的感染。然而,全面评估眼部暴露相对于呼吸道暴露如何影响病毒在哺乳动物中的致病性和传染性的研究有限,并且没有并排研究多种病毒家族。使用雪貂模型,我们发现,用多种冠状病毒或流感 A 病毒进行眼部暴露会导致感染,从而从接种动物中检测到可传播的气溶胶化病毒,从而导致两种病毒向易感接触者的传播。总的来说,这些研究支持眼部表面代表易受感染的黏膜表面,如果暴露于足够数量的病毒,就可以建立感染,其传染性与呼吸道暴露后相同。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c866/9769371/ace04d59545c/jvi.01403-22-f001.jpg

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