A recombinant subunit vaccine formulation protects against lethal Nipah virus challenge in cats

重组亚单位疫苗制剂可保护猫免受致命的尼帕病毒攻击

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作者:Jennifer A McEachern, John Bingham, Gary Crameri, Diane J Green, Tim J Hancock, Deborah Middleton, Yan-Ru Feng, Christopher C Broder, Lin-Fa Wang, Katharine N Bossart

Abstract

Nipah virus (NiV) and Hendra virus (HeV) are closely related deadly zoonotic paramyxoviruses that have emerged and re-emerged over the last 10 years. In this study, a subunit vaccine formulation containing only recombinant, soluble, attachment glycoprotein from HeV (sG(HeV)) and CpG adjuvant was evaluated as a potential NiV vaccine in the cat model. Different amounts of sG(HeV) were employed and sG-induced immunity was examined. Vaccinated animals demonstrated varying levels of NiV-specific Ig systemically and importantly, all vaccinated cats possessed antigen-specific IgA on the mucosa. Upon oronasal challenge with NiV (50,000TCID50), all vaccinated animals were protected from disease although virus was detected on day 21 post-challenge in one animal. The ability to elicit protective systemic and mucosal immunity in this animal model provides significant progress towards the development of a human subunit vaccine against henipaviruses.

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