A bivalent self-amplifying RNA vaccine against yellow fever and Zika viruses

Peter Battisti¹Matthew R Ykema¹Darshan N Kasal¹Madeleine Farber Jennewein¹Samuel Beaver¹Abbie E Weight²Derek Hanson³Jasneet Singh¹Julie Bakken¹Noah Cross¹Pauline Fusco¹Jacob Archer³Sierra Reed¹Alana Gerhardt¹Justin Grant Julander²Corey Casper¹Emily A Voigt^1*

• ¹Access to Advanced Health Institute, Seattle, United States
• ²Utah State University, Logan, Utah, United States
• ³Infectious Disease Research Institute, Seattle, Washington, United States

Introduction: Yellow fever (YFV) and Zika (ZIKV) viruses cause significant morbidity and mortality, despite the existence of an approved YFV vaccine and the development of multiple ZIKV vaccine candidates to date. New technologies may improve access to vaccines against these pathogens. We previously described a nanostructured lipid carrier (NLC)-delivered self-amplifying RNA (saRNA) vaccine platform with excellent thermostability and immunogenicity, appropriate for prevention of tropical infectious diseases.Methods: YFV and ZIKV prM-E antigen-expressing saRNA constructs were created using a TC-83 strain Venezuelan equine encephalitis virus-based replicon and complexed with NLC by simple mixing. Monovalent and bivalent vaccine formulations were injected intramuscularly into C57BL/6 mice and Syrian golden hamsters, and the magnitude, durability, and protective efficacy of the resulting immune responses were then characterized.Results and discussion: Monovalent vaccines established durable neutralizing antibody responses to their respective flaviviral targets, with little evidence of cross-neutralization. Both vaccines additionally elicited robust antigen-reactive CD4 + and CD8 + T cell populations. Notably, humoral responses to YFV saRNA-NLC vaccination were comparable to those in YF-17D-vaccinated animals. Bivalent formulations established humoral and cellular responses against both viral targets, commensurate to those established by monovalent vaccines, without evidence of saRNA interference or immune competition. Finally, both monovalent and bivalent vaccines completely protected mice and hamsters against lethal ZIKV and YFV challenge. We present a bivalent saRNA-NLC vaccine against YFV and ZIKV capable of inducing robust and efficacious neutralizing antibody and cellular immune responses against both viruses. These data support the development of other multivalent saRNA-based vaccines against infectious diseases.