Multivalent viral particles elicit safe and efficient immunoprotection against Nipah Hendra and Ebola viruses

Author:

Ithinji Duncan G.,Buchholz David W.ORCID,Ezzatpour Shahrzad,Monreal I. AbrreyORCID,Cong YuORCID,Sahler Julie,Bangar Amandip Singh,Imbiakha Brian,Upadhye Viraj,Liang Janie,Ma AndrewORCID,Bradel-Tretheway Birgit,Kaza Benjamin,Yeo Yao YuORCID,Choi Eun Jin,Johnston Gunner P.,Huzella Louis,Kollins Erin,Dixit Saurabh,Yu Shuiqing,Postnikova Elena,Ortega Victoria,August Avery,Holbrook Michael R.ORCID,Aguilar Hector C.ORCID

Abstract

AbstractExperimental vaccines for the deadly zoonotic Nipah (NiV), Hendra (HeV), and Ebola (EBOV) viruses have focused on targeting individual viruses, although their geographical and bat reservoir host overlaps warrant creation of multivalent vaccines. Here we explored whether replication-incompetent pseudotyped vesicular stomatitis virus (VSV) virions or NiV-based virus-like particles (VLPs) were suitable multivalent vaccine platforms by co-incorporating multiple surface glycoproteins from NiV, HeV, and EBOV onto these virions. We then enhanced the vaccines’ thermotolerance using carbohydrates to enhance applicability in global regions that lack cold-chain infrastructure. Excitingly, in a Syrian hamster model of disease, the VSV multivalent vaccine elicited safe, strong, and protective neutralizing antibody responses against challenge with NiV, HeV, or EBOV. Our study provides proof-of-principle evidence that replication-incompetent multivalent viral particle vaccines are sufficient to provide protection against multiple zoonotic deadly viruses with high pandemic potential.

Funder

United States Department of Defense | Defense Advanced Research Projects Agency

U.S. Department of Health & Human Services | NIH | National Institute of Allergy and Infectious Diseases

Publisher

Springer Science and Business Media LLC

Subject

Pharmacology (medical),Infectious Diseases,Pharmacology,Immunology

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