Unmodified rabies mRNA vaccine elicits high cross-neutralizing antibody titers and diverse B cell memory responses.
Fredrika HellgrenAlberto CagigiRodrigo Arcoverde CerveiraSebastian OlsTheresa KernAng LinBengt ErikssonMichael G DoddsEdith JasnyKim SchwendtConrad FreulingThomas MüllerMartin CorcoranGunilla B Karlsson HedestamBenjamin PetschKarin LoréPublished in: Nature communications (2023)
Licensed rabies virus vaccines based on whole inactivated virus are effective in humans. However, there is a lack of detailed investigations of the elicited immune response, and whether responses can be improved using novel vaccine platforms. Here we show that two doses of a lipid nanoparticle-formulated unmodified mRNA vaccine encoding the rabies virus glycoprotein (RABV-G) induces higher levels of RABV-G specific plasmablasts and T cells in blood, and plasma cells in the bone marrow compared to two doses of Rabipur in non-human primates. The mRNA vaccine also generates higher RABV-G binding and neutralizing antibody titers than Rabipur, while the degree of somatic hypermutation and clonal diversity of the response are similar for the two vaccines. The higher overall antibody titers induced by the mRNA vaccine translates into improved cross-neutralization of related lyssavirus strains, suggesting that this platform has potential for the development of a broadly protective vaccine against these viruses.
Keyphrases
- bone marrow
- immune response
- binding protein
- escherichia coli
- induced apoptosis
- dengue virus
- endothelial cells
- cell proliferation
- dendritic cells
- climate change
- high throughput
- working memory
- gene expression
- signaling pathway
- single cell
- zika virus
- fatty acid
- toll like receptor
- aedes aegypti
- transcription factor
- oxidative stress
- disease virus
- pluripotent stem cells