An optimized messenger RNA vaccine candidate protects non-human primates from Zika virus infection

Author:

Bollman Brooke,Nunna Naveen,Bahl Kapil,Hsiao Chiaowen JoyceORCID,Bennett Hamilton,Butler Scott,Foreman Bryant,Burgomaster Katherine E.,Aleshnick Maya,Kong Wing-Pui,Fisher Brian E.,Ruckwardt Tracy J.ORCID,Morabito Kaitlyn M.ORCID,Graham Barney S.,Dowd Kimberly A.,Pierson Theodore C.,Carfi Andrea

Abstract

AbstractZika virus (ZIKV), an arbovirus transmitted by mosquitoes, was identified as a cause of congenital disease during a major outbreak in the Americas in 2016. Vaccine design strategies relied on limited available isolate sequence information due to the rapid response necessary. The first-generation ZIKV mRNA vaccine, mRNA-1325, was initially generated and, as additional strain sequences became available, a second mRNA vaccine, mRNA-1893, was developed. Herein, we compared the immune responses following mRNA-1325 and mRNA-1893 vaccination and reported that mRNA-1893 generated comparable neutralizing antibody titers to mRNA-1325 at 1/20th of the dose and provided complete protection from ZIKV challenge in non-human primates. In-depth characterization of these vaccines indicated that the observed immunologic differences could be attributed to a single amino acid residue difference that compromised mRNA-1325 virus-like particle formation.

Publisher

Springer Science and Business Media LLC

Subject

Pharmacology (medical),Infectious Diseases,Pharmacology,Immunology

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