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与人类结膜炎相关的高致病性禽流感 A(H7N3)病毒的发病机制、传染性和眼倾向性。

Pathogenesis, transmissibility, and ocular tropism of a highly pathogenic avian influenza A (H7N3) virus associated with human conjunctivitis.

机构信息

Influenza Division, National Center for Immunization and Respiratory Diseases, Centers for Disease Control and Prevention, Atlanta, Georgia, USA.

出版信息

J Virol. 2013 May;87(10):5746-54. doi: 10.1128/JVI.00154-13. Epub 2013 Mar 13.

Abstract

H7 subtype influenza A viruses, responsible for numerous outbreaks in land-based poultry in Europe and the Americas, have caused over 100 cases of confirmed or presumed human infection over the last decade. The emergence of a highly pathogenic avian influenza H7N3 virus in poultry throughout the state of Jalisco, Mexico, resulting in two cases of human infection, prompted us to examine the virulence of this virus (A/Mexico/InDRE7218/2012 [MX/7218]) and related avian H7 subtype viruses in mouse and ferret models. Several high- and low-pathogenicity H7N3 and H7N9 viruses replicated efficiently in the respiratory tract of mice without prior adaptation following intranasal inoculation, but only MX/7218 virus caused lethal disease in this species. H7N3 and H7N9 viruses were also detected in the mouse eye following ocular inoculation. Virus from both H7N3 and H7N9 subtypes replicated efficiently in the upper and lower respiratory tracts of ferrets; however, only MX/7218 virus infection caused clinical signs and symptoms and was capable of transmission to naive ferrets in a direct-contact model. Similar to other highly pathogenic H7 viruses, MX/7218 replicated to high titers in human bronchial epithelial cells, yet it downregulated numerous genes related to NF-κB-mediated signaling transduction. These findings indicate that the recently isolated North American lineage H7 subtype virus associated with human conjunctivitis is capable of causing severe disease in mice and spreading to naive-contact ferrets, while concurrently retaining the ability to replicate within ocular tissue and allowing the eye to serve as a portal of entry.

摘要

H7 亚型流感病毒是造成欧洲和美洲陆生禽类多次暴发的元凶,在过去十年中已导致超过 100 例确诊或疑似人类感染病例。在墨西哥哈利斯科州,一种高致病性禽流感 H7N3 病毒在禽类中出现,导致 2 例人类感染病例,促使我们在小鼠和雪貂模型中检测这种病毒(A/Mexico/InDRE7218/2012 [MX/7218])及其相关的禽源 H7 亚型病毒的毒力。几种高致病性和低致病性 H7N3 和 H7N9 病毒在经鼻腔接种后无需预先适应,即可在小鼠呼吸道中高效复制,但只有 MX/7218 病毒可导致该物种发生致死性疾病。经眼部接种后,也可在小鼠眼部检测到 H7N3 和 H7N9 病毒。H7N3 和 H7N9 病毒也可在雪貂的上呼吸道和下呼吸道中高效复制;然而,只有 MX/7218 病毒感染可导致临床症状和体征,并可在直接接触模型中传播给无感染史的雪貂。与其他高致病性 H7 病毒类似,MX/7218 可在人支气管上皮细胞中高效复制,但它可下调许多与 NF-κB 介导的信号转导相关的基因。这些发现表明,与人类结膜炎相关的新近分离的北美谱系 H7 亚型病毒能够在小鼠中引起严重疾病并传播至无感染史的接触雪貂,同时保留在眼部组织中复制的能力并使眼睛成为入侵门户。

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