Safety and immunogenicity of a novel trivalent recombinant MVA-based equine encephalitis virus vaccine: A Phase 1 clinical trial

Carlos Fierro; Heinz Weidenthaler; Sanja Vidojkovic; Darja Schmidt; Zarina Gafoor; Daria Stroukova; Susan Zwiers; Jutta Müller; Ariane Volkmann

doi:10.1016/j.vaccine.2024.03.011

Safety and immunogenicity of a novel trivalent recombinant MVA-based equine encephalitis virus vaccine: A Phase 1 clinical trial

Vaccine. 2024 Apr 11;42(10):2695-2706. doi: 10.1016/j.vaccine.2024.03.011. Epub 2024 Mar 16.

Authors

Carlos Fierro¹, Heinz Weidenthaler², Sanja Vidojkovic², Darja Schmidt², Zarina Gafoor³, Daria Stroukova², Susan Zwiers³, Jutta Müller⁴, Ariane Volkmann⁵

Affiliations

¹ Johnson County Clin-Trials (JCCT), 16400 College Blvd., Lenexa, KS 66219, USA.
² Bavarian Nordic GmbH, Fraunhoferstrasse 13, 82152 Martinsried, Germany.
³ Bavarian Nordic Inc, 1005 Slater Road, Suite 101, Durham, NC 27703, USA.
⁴ Immunic AG, Lochhamer Schlag 21, 82166 Gräfelfing, Germany.
⁵ Bavarian Nordic GmbH, Fraunhoferstrasse 13, 82152 Martinsried, Germany. Electronic address: Ariane.Volkmann@bavarian-nordic.com.

PMID: 38494412
DOI: 10.1016/j.vaccine.2024.03.011

Abstract

Background: Three encephalitic alphaviruses-western, eastern, and Venezuelan equine encephalitis virus (WEEV, EEEV and VEEV)-can cause severe disease and have the potential to be used as biological weapons. There are no approved vaccines for human use. A novel multivalent MVA-BN-WEV vaccine encodes the envelope surface proteins of the 3 viruses and is thereby potentially able to protect against them all, as previously demonstrated in animal models. This first-in-human study assessed the safety, tolerability, and immunogenicity of MVA-BN-WEV vaccine in healthy adult participants.

Methods: Forty-five participants were enrolled into 3 dose groups (1 × 10E7 Inf.U, 1 × 10E8 Inf.U, and 2 × 10E8 Inf.U), received 2 doses 4 weeks apart, and were then monitored for 6 months.

Results: The safety profile of MVA-BN-WEV was acceptable at all administered doses, with incidence of local solicited AEs increased with increasing dose and no other clinically meaningful differences between dose groups. One SAE (Grade 2 pleural effusion) was reported in the lowest dose group and assessed as possibly related. No AEs resulted in death or led to withdrawal from the second vaccination or from the trial. The most common local solicited AE was injection site pain, and general solicited AEs were headache, fatigue, and myalgia. MVA-BN-WEV induced humoral immune responses; WEEV-, EEEV- and VEEV-specific neutralizing antibody responses peaked 2 weeks following the second vaccination, and the magnitude of these responses increased with dose escalation. The highest dose resulted in seroconversion of all (100 %) participants for WEEV and VEEV and 92.9 % for EEEV, 2 weeks following second vaccination, and durability was observed for 6 months. MVA-BN-WEV induced cellular immune responses to VEEV E1 and E2 (EEEV and WEEV not tested) and a dose effect for peptide pool E2.

Conclusion: The study demonstrated that MVA-BN-WEV is well tolerated, induces immune responses, and is suitable for further development.

Clinical trial registry number: NCT04131595.

Keywords: Alphavirus; Eastern equine encephalitis virus (EEEV); Encephalitis; MVA; Vaccine; Venezuelan equine encephalitis virus (VEEV); Western equine encephalitis virus (WEEV).

Publication types

Clinical Trial, Phase I

MeSH terms

Alphavirus*
Animals
Antibodies, Neutralizing
Antibodies, Viral
Encephalitis Virus, Venezuelan Equine*
Encephalomyelitis, Equine* / prevention & control
Horses
Humans
Immunogenicity, Vaccine
Vaccinia virus

Substances

Antibodies, Viral
Antibodies, Neutralizing

Associated data

ClinicalTrials.gov/NCT04131595