Multivalent mRNA-DTP vaccines are immunogenic and provide protection from Bordetella pertussis challenge in mice

Author:

Wolf M. Allison,O’Hara Joanne M.,Bitzer Graham J.ORCID,Narayanan Elisabeth,Boehm Dylan T.ORCID,Bevere Justin R.,DeJong Megan A.,Hall Jesse M.,Wong Ting Y.,Falcone Samantha,Deal Cailin E.,Richards Angelene,Green Shannon,Nguyen Brenda,King Emily,Ogega ClintonORCID,Russo Lisa,Sen-Kilic EmelORCID,Plante Obadiah,Himansu SunnyORCID,Barbier MarietteORCID,Carfi Andrea,Damron F. HeathORCID

Abstract

AbstractAcellular multivalent vaccines for pertussis (DTaP and Tdap) prevent symptomatic disease and infant mortality, but immunity to Bordetella pertussis infection wanes significantly over time resulting in cyclic epidemics of pertussis. The messenger RNA (mRNA) vaccine platform provides an opportunity to address complex bacterial infections with an adaptable approach providing Th1-biased responses. In this study, immunogenicity and challenge models were used to evaluate the mRNA platform with multivalent vaccine formulations targeting both B. pertussis antigens and diphtheria and tetanus toxoids. Immunization with mRNA formulations were immunogenetic, induced antigen specific antibodies, as well as Th1 T cell responses. Upon challenge with either historical or contemporary B. pertussis strains, 6 and 10 valent mRNA DTP vaccine provided protection equal to that of 1/20th human doses of either DTaP or whole cell pertussis vaccines. mRNA DTP immunized mice were also protected from pertussis toxin challenge as measured by prevention of lymphocytosis and leukocytosis. Collectively these pre-clinical mouse studies illustrate the potential of the mRNA platform for multivalent bacterial pathogen vaccines.

Funder

U.S. Department of Health & Human Services | NIH | National Institute of Allergy and Infectious Diseases

Publisher

Springer Science and Business Media LLC

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