Mutation-guided vaccine design: A process for developing boosting immunogens for HIV broadly neutralizing antibody induction.

A major goal of HIV-1 vaccine development is the induction of broadly neutralizing antibodies (bnAbs). Although success has been achieved in initiating bnAb B cell lineages, design of boosting immunogens that select for bnAb B cell receptors with improbable mutations required for bnAb affinity maturation remains difficult. Here, we demonstrate a process for designing boosting immunogens for a V3-glycan bnAb B cell lineage. The immunogens induced affinity-matured antibodies by selecting for functional improbable mutations in bnAb precursor knockin mice. Moreover, we show similar success in prime and boosting with nucleoside-modified mRNA-encoded HIV-1 envelope trimer immunogens, with improved selection by mRNA immunogens of improbable mutations required for bnAb binding to key envelope glycans. These results demonstrate the ability of both protein and mRNA prime-boost immunogens for selection of rare B cell lineage intermediates with neutralizing breadth after bnAb precursor expansion, a key proof of concept and milestone toward development of an HIV-1 vaccine.

Duke Scholars

Author Wilton Bryan Williams Surgery, Surgical Sciences

Author S. Munir Alam Medicine, Duke Human Vaccine Institute

Author Kevin J Wiehe Medicine, Duke Human Vaccine Institute

Author Kevin O'Neil Saunders Surgery, Surgical Sciences

Author Derek Wilson Cain Medicine, Duke Human Vaccine Institute

Author Rory Henderson Medicine, Duke Human Vaccine Institute

Author David Charles Montefiori Surgery, Surgical Sciences

Author Priyamvada Acharya Surgery, Surgical Sciences

Author Barton Ford Haynes Medicine, Duke Human Vaccine Institute