Safety Concern of Recombination Between Self-amplifying MRNA Vaccines and Viruses is Mitigated In vivo

Overview

Journal Mol Ther

Publisher Cell Press

Specialties Molecular Biology
Pharmacology

Date 2024 Jun 19

PMID 38894543

Authors

Tessy A H Hick

Corinne Geertsema

Wilson Nguyen

Cameron R Bishop

Linda van Oosten

Sandra R Abbo

Troy Dumenil

Frank J M van Kuppeveld

Martijn A Langereis

Daniel J Rawle

Bing Tang

Kexin Yan

Monique M van Oers

Andreas Suhrbier

Gorben P Pijlman

Affiliations

Soon will be listed here.

Abstract

Self-amplifying mRNA (SAM) vaccines can be rapidly deployed in the event of disease outbreaks. A legitimate safety concern is the potential for recombination between alphavirus-based SAM vaccines and circulating viruses. This theoretical risk needs to be assessed in the regulatory process for SAM vaccine approval. Herein, we undertake extensive in vitro and in vivo assessments to explore recombination between SAM vaccine and a wide selection of alphaviruses and a coronavirus. SAM vaccines were found to effectively limit alphavirus co-infection through superinfection exclusion, although some co-replication was still possible. Using sensitive cell-based assays, replication-competent alphavirus chimeras were generated in vitro as a result of rare, but reproducible, RNA recombination events. The chimeras displayed no increased fitness in cell culture. Viable alphavirus chimeras were not detected in vivo in C57BL/6J, Rag1 and Ifnar mice, in which high levels of SAM vaccine and alphavirus co-replicated in the same tissue. Furthermore, recombination between a SAM-spike vaccine and a swine coronavirus was not observed. In conclusion we state that although the ability of SAM vaccines to recombine with alphaviruses might be viewed as an environmental safety concern, several key factors substantially mitigate against in vivo emergence of chimeric viruses from SAM vaccine recipients.

Citing Articles

Can self-amplifying RNA vaccines and viruses exchange genetic material?.

Casmil I, Blakney A Mol Ther. 2024; 32(8):2437-2438.

PMID: 39032486 PMC: 11405170. DOI: 10.1016/j.ymthe.2024.07.003.

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