Deep phenotypic characterization of immunization-induced antibacterial IgG repertoires in mice using a single-antibody bioassay - Archive ouverte HAL Access content directly
Journal Articles Communications Biology Year : 2020

Deep phenotypic characterization of immunization-induced antibacterial IgG repertoires in mice using a single-antibody bioassay

Abstract

Antibodies with antibacterial activity need to bind to the bacterial surface with affinity, specificity, and sufficient density to induce efficient elimination. To characterize the antibacterial antibody repertoire, we developed an in-droplet bioassay with single-antibody resolution. The assay not only allowed us to identify whether the secreted antibodies recognized a bacterial surface antigen, but also to estimate the apparent dissociation constant (K D app) of the interaction and the density of the recognized epitope on the bacteria. Herein, we found substantial differences within the K D app /epitope density profiles in mice immunized with various species of heat-killed bacteria. The experiments further revealed a high cross-reactivity of the secreted IgG repertoires, binding to even unrelated bacteria with high affinity. This application confirmed the ability to quantify the anti-bacterial antibody repertoire and the utility of the developed bioassay to study the interplay between bacteria and the humoral response.
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hal-03054253 , version 1 (16-12-2020)

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Millie Heo, Guilhem Chenon, Carlos Castrillon, Jérôme Bibette, Pierre Bruhns, et al.. Deep phenotypic characterization of immunization-induced antibacterial IgG repertoires in mice using a single-antibody bioassay. Communications Biology, 2020, 3 (1), pp.614. ⟨10.1038/s42003-020-01296-3⟩. ⟨hal-03054253⟩
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