Delayed reinforcement of costimulation improves the efficacy of mRNA vaccines in mice

免疫学 钢筋 医学 信使核糖核酸 病毒学 生物 心理学 遗传学 社会心理学 基因
作者
Sarah Sanchez,Tanushree Dangi,Bakare Awakoaiye,Min Han Lew,Nahid Irani,Slim Fourati,Pablo Penaloza‐MacMaster
出处
期刊:Journal of Clinical Investigation [American Society for Clinical Investigation]
标识
DOI:10.1172/jci183973
摘要

mRNA vaccines have demonstrated efficacy during the COVID-19 pandemic and are now being investigated for multiple diseases. However, concerns linger about the durability of immune responses, and the high incidence of breakthrough infections among vaccinated individuals highlights the need for improved mRNA vaccines. In this study, we investigated the effects of reinforcing costimulation via 4-1BB, a member of the TNF receptor superfamily, on immune responses elicited by mRNA vaccines. We first immunized mice with mRNA vaccines, followed by treatment with 4-1BB costimulatory antibodies to reinforce the 4-1BB pathway at different timepoints post-vaccination. Consistent with prior studies, reinforcing 4-1BB costimulation on the day of vaccination did not result in a substantial improvement of vaccine responses. However, reinforcing 4-1BB costimulation at day 4 post-vaccination, when 4-1BB expression levels were highest, resulted in a profound improvement of CD8 T cell responses associated with enhanced protection against pathogen challenges. A similar clinical benefit was observed in a therapeutic cancer vaccine model. We also report time-dependent effects with OX40, another costimulatory molecule of the TNF receptor superfamily. These findings demonstrate that delayed reinforcement of costimulation may exert an immunologic benefit, providing insights for the development of more effective mRNA vaccines for infectious diseases and cancer.

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