TY - JOUR TI - Binding affinity landscapes constrain the evolution of broadly neutralizing anti-influenza antibodies AU - Phillips, Angela M AU - Lawrence, Katherine R AU - Moulana, Alief AU - Dupic, Thomas AU - Chang, Jeffrey AU - Johnson, Milo S AU - Cvijovic, Ivana AU - Mora, Thierry AU - Walczak, Aleksandra M AU - Desai, Michael M A2 - Fleishman, Sarel Jacob A2 - Rath, Satyajit A2 - Bloom, Jesse D A2 - Wu, Nicholas C VL - 10 PY - 2021 DA - 2021/09/07 SP - e71393 C1 - eLife 2021;10:e71393 DO - 10.7554/eLife.71393 UR - https://doi.org/10.7554/eLife.71393 AB - Over the past two decades, several broadly neutralizing antibodies (bnAbs) that confer protection against diverse influenza strains have been isolated. Structural and biochemical characterization of these bnAbs has provided molecular insight into how they bind distinct antigens. However, our understanding of the evolutionary pathways leading to bnAbs, and thus how best to elicit them, remains limited. Here, we measure equilibrium dissociation constants of combinatorially complete mutational libraries for two naturally isolated influenza bnAbs (CR9114, 16 heavy-chain mutations; CR6261, 11 heavy-chain mutations), reconstructing all possible evolutionary intermediates back to the unmutated germline sequences. We find that these two libraries exhibit strikingly different patterns of breadth: while many variants of CR6261 display moderate affinity to diverse antigens, those of CR9114 display appreciable affinity only in specific, nested combinations. By examining the extensive pairwise and higher order epistasis between mutations, we find key sites with strong synergistic interactions that are highly similar across antigens for CR6261 and different for CR9114. Together, these features of the binding affinity landscapes strongly favor sequential acquisition of affinity to diverse antigens for CR9114, while the acquisition of breadth to more similar antigens for CR6261 is less constrained. These results, if generalizable to other bnAbs, may explain the molecular basis for the widespread observation that sequential exposure favors greater breadth, and such mechanistic insight will be essential for predicting and eliciting broadly protective immune responses. KW - influenza KW - antibody KW - landscape KW - evolution KW - epistasis KW - breadth JF - eLife SN - 2050-084X PB - eLife Sciences Publications, Ltd ER -