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用颗粒介导的甲型流感病毒DNA疫苗免疫猪可使其免受同源病毒攻击。

Immunization of pigs with a particle-mediated DNA vaccine to influenza A virus protects against challenge with homologous virus.

作者信息

Macklin M D, McCabe D, McGregor M W, Neumann V, Meyer T, Callan R, Hinshaw V S, Swain W F

机构信息

PowderJect Vaccines, Inc., Madison, Wisconsin 53711, USA.

出版信息

J Virol. 1998 Feb;72(2):1491-6. doi: 10.1128/JVI.72.2.1491-1496.1998.

DOI:10.1128/JVI.72.2.1491-1496.1998
PMID:9445052
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC124630/
Abstract

Particle-mediated delivery of a DNA expression vector encoding the hemagglutinin (HA) of an H1N1 influenza virus (A/Swine/Indiana/1726/88) to porcine epidermis elicits a humoral immune response and accelerates the clearance of virus in pigs following a homotypic challenge. Mucosal administration of the HA expression plasmid elicits an immune response that is qualitatively different than that elicited by the epidermal vaccination in terms of inhibition of the initial virus infection. In contrast, delivery of a plasmid encoding an influenza virus nucleoprotein from A/PR/8/34 (H1N1) to the epidermis elicits a strong humoral response but no detectable protection in terms of nasal virus shed. The efficacy of the HA DNA vaccine was compared with that of a commercially available inactivated whole-virus vaccine as well as with the level of immunity afforded by previous infection. The HA DNA and inactivated viral vaccines elicited similar protection in that initial infection was not prevented, but subsequent amplification of the infection is limited, resulting in early clearance of the virus. Convalescent animals which recovered from exposure to virulent swine influenza virus were completely resistant to infection when challenged. The porcine influenza A virus system is a relevant preclinical model for humans in terms of both disease and gene transfer to the epidermis and thus provides a basis for advancing the development of DNA-based vaccines.

摘要

将编码H1N1流感病毒(A/猪/印第安纳/1726/88)血凝素(HA)的DNA表达载体通过颗粒介导的方式递送至猪表皮,可引发体液免疫反应,并在同型攻击后加速猪体内病毒的清除。HA表达质粒的黏膜给药引发的免疫反应在抑制初始病毒感染方面与表皮疫苗接种引发的免疫反应在性质上有所不同。相比之下,将编码来自A/PR/8/34(H1N1)的流感病毒核蛋白的质粒递送至表皮会引发强烈的体液反应,但在鼻病毒排出方面未检测到保护作用。将HA DNA疫苗的效力与市售灭活全病毒疫苗的效力以及先前感染所提供的免疫水平进行了比较。HA DNA疫苗和灭活病毒疫苗引发了相似的保护作用,即虽然不能预防初始感染,但可限制感染的后续扩增,从而导致病毒的早期清除。从接触强毒性猪流感病毒中恢复的恢复期动物在受到攻击时对感染具有完全抵抗力。就疾病以及向表皮的基因转移而言,猪甲型流感病毒系统是人类相关的临床前模型,因此为推进基于DNA的疫苗开发提供了基础。

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