Polymeric and lipid nanoparticles for delivery of self-amplifying RNA vaccines

免疫原性 生物 核糖核酸 病毒学 接种疫苗 微生物学 抗原 免疫学 基因 生物化学
作者
Anna K. Blakney,Paul F. McKay,Kai Hu,Karnyart Samnuan,Nikita Jain,Andrew F. Brown,A.M. Thomas,Paul Rogers,Krunal Polra,Hadijatou Sallah,Jonathan Yeow,Yunqing Zhu,Molly M. Stevens,Andrew J. Geall,Robin J. Shattock
出处
期刊:Journal of Controlled Release [Elsevier BV]
卷期号:338: 201-210 被引量:106
标识
DOI:10.1016/j.jconrel.2021.08.029
摘要

Self-amplifying RNA (saRNA) is a next-generation vaccine platform, but like all nucleic acids, requires a delivery vehicle to promote cellular uptake and protect the saRNA from degradation. To date, delivery platforms for saRNA have included lipid nanoparticles (LNP), polyplexes and cationic nanoemulsions; of these LNP are the most clinically advanced with the recent FDA approval of COVID-19 based-modified mRNA vaccines. While the effect of RNA on vaccine immunogenicity is well studied, the role of biomaterials in saRNA vaccine effectiveness is under investigated. Here, we tested saRNA formulated with either pABOL, a bioreducible polymer, or LNP, and characterized the protein expression and vaccine immunogenicity of both platforms. We observed that pABOL-formulated saRNA resulted in a higher magnitude of protein expression, but that the LNP formulations were overall more immunogenic. Furthermore, we observed that both the helper phospholipid and route of administration (intramuscular versus intranasal) of LNP impacted the vaccine immunogenicity of two model antigens (influenza hemagglutinin and SARS-CoV-2 spike protein). We observed that LNP administered intramuscularly, but not pABOL or LNP administered intranasally, resulted in increased acute interleukin-6 expression after vaccination. Overall, these results indicate that delivery systems and routes of administration may fulfill different delivery niches within the field of saRNA genetic medicines.
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