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生成和鉴定一种适应寒冷环境的减毒活 H3N2 亚型流感病毒候选疫苗。

Generation and characterization of a cold-adapted attenuated live H3N2 subtype influenza virus vaccine candidate.

机构信息

College of Animal Science and Veterinary Medicine, Jilin University, Changchun, Jilin, China.

出版信息

Chin Med J (Engl). 2009 Dec 5;122(23):2880-5.

Abstract

BACKGROUND

H3N2 subtype influenza A viruses have been identified in humans worldwide, raising concerns about their pandemic potential and prompting the development of candidate vaccines to protect humans against this subtype of influenza A virus. The aim of this study was to establish a system for rescuing of a cold-adapted high-yielding H3N2 subtype human influenza virus by reverse genetics.

METHODS

In order to generate better and safer vaccine candidate viruses, a cold-adapted high yielding reassortant H3N2 influenza A virus was genetically constructed by reverse genetics and was designated as rgAA-H3N2. The rgAA-H3N2 virus contained HA and NA genes from an epidemic strain A/Wisconsin/67/2005 (H3N2) in a background of internal genes derived from the master donor viruses (MDV), cold-adapted (ca), temperature sensitive (ts), live attenuated influenza virus strain A/Ann Arbor/6/60 (MDV-A).

RESULTS

In this presentation, the virus HA titer of rgAA-H3N2 in the allantoic fluid from infected embryonated eggs was as high as 1:1024. A fluorescent focus assay (FFU) was performed 24-36 hours post-infection using a specific antibody and bright staining was used for determining the virus titer. The allantoic fluid containing the recovered influenza virus was analyzed in a hemagglutination inhibition (HI) test and the specific inhibition was found.

CONCLUSION

The results mentioned above demonstrated that cold-adapted, attenuated reassortant H3N2 subtype influenza A virus was successfully generated, which laid a good foundation for the further related research.

摘要

背景

H3N2 亚型流感 A 病毒已在全球范围内被发现,引起了人们对其大流行潜力的关注,并促使开发候选疫苗以保护人类免受这种亚型流感 A 病毒的侵害。本研究旨在建立一种通过反向遗传学拯救冷适应高产 H3N2 亚型人流感病毒的系统。

方法

为了生成更好、更安全的疫苗候选病毒,通过反向遗传学构建了一种冷适应高产重配 H3N2 流感 A 病毒,并将其命名为 rgAA-H3N2。rgAA-H3N2 病毒的 HA 和 NA 基因来自流行株 A/Wisconsin/67/2005(H3N2),内部基因来自主供体病毒(MDV),冷适应(ca),温度敏感(ts),活减毒流感病毒株 A/Ann Arbor/6/60(MDV-A)。

结果

在本研究中,rgAA-H3N2 在感染鸡胚的尿囊液中的病毒 HA 滴度高达 1:1024。感染后 24-36 小时通过特异性抗体进行荧光焦点测定(FFU),并使用明亮染色来确定病毒滴度。对回收的流感病毒进行血凝抑制(HI)试验,发现具有特定抑制作用。

结论

上述结果表明,成功生成了冷适应、减毒的重配 H3N2 亚型流感 A 病毒,为进一步的相关研究奠定了良好的基础。

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