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Large-scale antibody immune response mapping of splenic B cells and bone marrow plasma cells in a transgenic mouse model

Molecular characterization of antibody immunity and human antibody discovery is mainly carried out using peripheral memory B cells, and occasionally plasmablasts, that express B cell receptors (BCRs) on their cell surface. Despite the importance of plasma cells (PCs) as the dominant source of circul...

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Autores principales: Pan, Xiaoli, López Acevedo, Sheila N., Cuziol, Camille, De Tavernier, Evelyn, Fahad, Ahmed S., Longjam, Priyobarta S., Rao, Sambasiva P., Aguilera-Rodríguez, David, Rezé, Mathilde, Bricault, Christine A., Gutiérrez-González, Matías F., de Souza, Matheus Oliveira, DiNapoli, Joshua M., Vigne, Emmanuelle, Shahsavarian, Melody A., DeKosky, Brandon J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10280637/
https://www.ncbi.nlm.nih.gov/pubmed/37346047
http://dx.doi.org/10.3389/fimmu.2023.1137069
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author Pan, Xiaoli
López Acevedo, Sheila N.
Cuziol, Camille
De Tavernier, Evelyn
Fahad, Ahmed S.
Longjam, Priyobarta S.
Rao, Sambasiva P.
Aguilera-Rodríguez, David
Rezé, Mathilde
Bricault, Christine A.
Gutiérrez-González, Matías F.
de Souza, Matheus Oliveira
DiNapoli, Joshua M.
Vigne, Emmanuelle
Shahsavarian, Melody A.
DeKosky, Brandon J.
author_facet Pan, Xiaoli
López Acevedo, Sheila N.
Cuziol, Camille
De Tavernier, Evelyn
Fahad, Ahmed S.
Longjam, Priyobarta S.
Rao, Sambasiva P.
Aguilera-Rodríguez, David
Rezé, Mathilde
Bricault, Christine A.
Gutiérrez-González, Matías F.
de Souza, Matheus Oliveira
DiNapoli, Joshua M.
Vigne, Emmanuelle
Shahsavarian, Melody A.
DeKosky, Brandon J.
author_sort Pan, Xiaoli
collection PubMed
description Molecular characterization of antibody immunity and human antibody discovery is mainly carried out using peripheral memory B cells, and occasionally plasmablasts, that express B cell receptors (BCRs) on their cell surface. Despite the importance of plasma cells (PCs) as the dominant source of circulating antibodies in serum, PCs are rarely utilized because they do not express surface BCRs and cannot be analyzed using antigen-based fluorescence-activated cell sorting. Here, we studied the antibodies encoded by the entire mature B cell populations, including PCs, and compared the antibody repertoires of bone marrow and spleen compartments elicited by immunization in a human immunoglobulin transgenic mouse strain. To circumvent prior technical limitations for analysis of plasma cells, we applied single-cell antibody heavy and light chain gene capture from the entire mature B cell repertoires followed by yeast display functional analysis using a cytokine as a model immunogen. We performed affinity-based sorting of antibody yeast display libraries and large-scale next-generation sequencing analyses to follow antibody lineage performance, with experimental validation of 76 monoclonal antibodies against the cytokine antigen that identified three antibodies with exquisite double-digit picomolar binding affinity. We observed that spleen B cell populations generated higher affinity antibodies compared to bone marrow PCs and that antigen-specific splenic B cells had higher average levels of somatic hypermutation. A degree of clonal overlap was also observed between bone marrow and spleen antibody repertoires, indicating common origins of certain clones across lymphoid compartments. These data demonstrate a new capacity to functionally analyze antigen-specific B cell populations of different lymphoid organs, including PCs, for high-affinity antibody discovery and detailed fundamental studies of antibody immunity.
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spelling pubmed-102806372023-06-21 Large-scale antibody immune response mapping of splenic B cells and bone marrow plasma cells in a transgenic mouse model Pan, Xiaoli López Acevedo, Sheila N. Cuziol, Camille De Tavernier, Evelyn Fahad, Ahmed S. Longjam, Priyobarta S. Rao, Sambasiva P. Aguilera-Rodríguez, David Rezé, Mathilde Bricault, Christine A. Gutiérrez-González, Matías F. de Souza, Matheus Oliveira DiNapoli, Joshua M. Vigne, Emmanuelle Shahsavarian, Melody A. DeKosky, Brandon J. Front Immunol Immunology Molecular characterization of antibody immunity and human antibody discovery is mainly carried out using peripheral memory B cells, and occasionally plasmablasts, that express B cell receptors (BCRs) on their cell surface. Despite the importance of plasma cells (PCs) as the dominant source of circulating antibodies in serum, PCs are rarely utilized because they do not express surface BCRs and cannot be analyzed using antigen-based fluorescence-activated cell sorting. Here, we studied the antibodies encoded by the entire mature B cell populations, including PCs, and compared the antibody repertoires of bone marrow and spleen compartments elicited by immunization in a human immunoglobulin transgenic mouse strain. To circumvent prior technical limitations for analysis of plasma cells, we applied single-cell antibody heavy and light chain gene capture from the entire mature B cell repertoires followed by yeast display functional analysis using a cytokine as a model immunogen. We performed affinity-based sorting of antibody yeast display libraries and large-scale next-generation sequencing analyses to follow antibody lineage performance, with experimental validation of 76 monoclonal antibodies against the cytokine antigen that identified three antibodies with exquisite double-digit picomolar binding affinity. We observed that spleen B cell populations generated higher affinity antibodies compared to bone marrow PCs and that antigen-specific splenic B cells had higher average levels of somatic hypermutation. A degree of clonal overlap was also observed between bone marrow and spleen antibody repertoires, indicating common origins of certain clones across lymphoid compartments. These data demonstrate a new capacity to functionally analyze antigen-specific B cell populations of different lymphoid organs, including PCs, for high-affinity antibody discovery and detailed fundamental studies of antibody immunity. Frontiers Media S.A. 2023-06-05 /pmc/articles/PMC10280637/ /pubmed/37346047 http://dx.doi.org/10.3389/fimmu.2023.1137069 Text en Copyright © 2023 Pan, López Acevedo, Cuziol, De Tavernier, Fahad, Longjam, Rao, Aguilera-Rodríguez, Rezé, Bricault, Gutiérrez-González, de Souza, DiNapoli, Vigne, Shahsavarian and DeKosky https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Pan, Xiaoli
López Acevedo, Sheila N.
Cuziol, Camille
De Tavernier, Evelyn
Fahad, Ahmed S.
Longjam, Priyobarta S.
Rao, Sambasiva P.
Aguilera-Rodríguez, David
Rezé, Mathilde
Bricault, Christine A.
Gutiérrez-González, Matías F.
de Souza, Matheus Oliveira
DiNapoli, Joshua M.
Vigne, Emmanuelle
Shahsavarian, Melody A.
DeKosky, Brandon J.
Large-scale antibody immune response mapping of splenic B cells and bone marrow plasma cells in a transgenic mouse model
title Large-scale antibody immune response mapping of splenic B cells and bone marrow plasma cells in a transgenic mouse model
title_full Large-scale antibody immune response mapping of splenic B cells and bone marrow plasma cells in a transgenic mouse model
title_fullStr Large-scale antibody immune response mapping of splenic B cells and bone marrow plasma cells in a transgenic mouse model
title_full_unstemmed Large-scale antibody immune response mapping of splenic B cells and bone marrow plasma cells in a transgenic mouse model
title_short Large-scale antibody immune response mapping of splenic B cells and bone marrow plasma cells in a transgenic mouse model
title_sort large-scale antibody immune response mapping of splenic b cells and bone marrow plasma cells in a transgenic mouse model
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10280637/
https://www.ncbi.nlm.nih.gov/pubmed/37346047
http://dx.doi.org/10.3389/fimmu.2023.1137069
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