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甲型流感病毒H6减毒活疫苗在小鼠和雪貂中的评估。

Evaluation of live attenuated influenza a virus h6 vaccines in mice and ferrets.

作者信息

Chen Zhongying, Santos Celia, Aspelund Amy, Gillim-Ross Laura, Jin Hong, Kemble George, Subbarao Kanta

机构信息

Laboratory of Infectious Diseases, NIAID, NIH, Bldg. 33/Room 3E13C.1, 33 North Dr., MSC 3203, Bethesda, MD 20892, USA.

出版信息

J Virol. 2009 Jan;83(1):65-72. doi: 10.1128/JVI.01775-08. Epub 2008 Oct 22.

Abstract

Avian influenza A virus A/teal/HK/W312/97 (H6N1) possesses seven gene segments that are highly homologous to those of highly pathogenic human influenza H5N1 viruses, suggesting that a W312-like H6N1 virus might have been involved in the generation of the A/HK/97 H5N1 viruses. The continuous circulation and reassortment of influenza H6 subtype viruses in birds highlight the need to develop an H6 vaccine to prevent potential influenza pandemics caused by the H6 viruses. Based on the serum antibody cross-reactivity data obtained from 14 different H6 viruses from Eurasian and North American lineages, A/duck/HK/182/77, A/teal/HK/W312/97, and A/mallard/Alberta/89/85 were selected to produce live attenuated H6 candidate vaccines. Each of the H6 vaccine strains is a 6:2 reassortant ca virus containing HA and NA gene segments from an H6 virus and the six internal gene segments from cold-adapted A/Ann Arbor/6/60 (AA ca), the master donor virus that is used to make live attenuated influenza virus FluMist (intranasal) vaccine. All three H6 vaccine candidates exhibited phenotypic properties of temperature sensitivity (ts), ca, and attenuation (att) conferred by the internal gene segments from AA ca. Intranasal administration of a single dose of the three H6 ca vaccine viruses induced neutralizing antibodies in mice and ferrets and fully protected mice and ferrets from homologous wild-type (wt) virus challenge. Among the three H6 vaccine candidates, the A/teal/HK/W312/97 ca virus provided the broadest cross-protection against challenge with three antigenically distinct H6 wt viruses. These data support the rationale for further evaluating the A/teal/HK/W312/97 ca vaccine in humans.

摘要

甲型禽流感病毒A/绿头鸭/香港/W312/97(H6N1)拥有7个基因片段,这些片段与高致病性人类流感H5N1病毒的基因片段高度同源,这表明类似W312的H6N1病毒可能参与了A/香港/97 H5N1病毒的产生。H6亚型流感病毒在鸟类中的持续传播和重配突出了开发H6疫苗以预防由H6病毒引起的潜在流感大流行的必要性。根据从欧亚和北美谱系的14种不同H6病毒获得的血清抗体交叉反应数据,选择A/鸭/香港/182/77、A/绿头鸭/香港/W312/97和A/野鸭/艾伯塔/89/85来生产减毒活H6候选疫苗。每种H6疫苗株都是一种6:2重配的ca病毒,包含来自H6病毒的HA和NA基因片段以及来自冷适应的A/安阿伯/6/60(AA ca)的六个内部基因片段,AA ca是用于生产减毒活流感病毒FluMist(鼻内)疫苗的主供体病毒。所有三种H6候选疫苗都表现出由AA ca的内部基因片段赋予的温度敏感性(ts)、冷适应(ca)和减毒(att)的表型特性。单剂量鼻内接种三种H6 ca疫苗病毒可在小鼠和雪貂中诱导中和抗体,并能完全保护小鼠和雪貂免受同源野生型(wt)病毒的攻击。在三种H6候选疫苗中,A/绿头鸭/香港/W312/97 ca病毒对三种抗原性不同的H6 wt病毒攻击提供了最广泛的交叉保护。这些数据支持了在人体中进一步评估A/绿头鸭/香港/W312/97 ca疫苗的理论依据。

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