Application of B cell immortalization for the isolation of antibodies and B cell clones from vaccine and infection settings

The isolation and characterization of neutralizing antibodies from infection and vaccine settings informs future vaccine design, and methodologies that streamline the isolation of antibodies and the generation of B cell clones are of great interest. Retroviral transduction to express Bcl-6 and Bcl-x...

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Autores principales: Boswell, Kristin L., Watkins, Timothy A., Cale, Evan M., Samsel, Jakob, Andrews, Sarah F., Ambrozak, David R., Driscoll, Jefferson I., Messina, Michael A., Narpala, Sandeep, Hopp, Christine S., Cagigi, Alberto, Casazza, Joseph P., Yamamoto, Takuya, Zhou, Tongqing, Schief, William R., Crompton, Peter D., Ledgerwood, Julie E., Connors, Mark, Gama, Lucio, Kwong, Peter D., McDermott, Adrian, Mascola, John R., Koup, Richard A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9794141/
https://www.ncbi.nlm.nih.gov/pubmed/36582240
http://dx.doi.org/10.3389/fimmu.2022.1087018
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author Boswell, Kristin L.
Watkins, Timothy A.
Cale, Evan M.
Samsel, Jakob
Andrews, Sarah F.
Ambrozak, David R.
Driscoll, Jefferson I.
Messina, Michael A.
Narpala, Sandeep
Hopp, Christine S.
Cagigi, Alberto
Casazza, Joseph P.
Yamamoto, Takuya
Zhou, Tongqing
Schief, William R.
Crompton, Peter D.
Ledgerwood, Julie E.
Connors, Mark
Gama, Lucio
Kwong, Peter D.
McDermott, Adrian
Mascola, John R.
Koup, Richard A.
author_facet Boswell, Kristin L.
Watkins, Timothy A.
Cale, Evan M.
Samsel, Jakob
Andrews, Sarah F.
Ambrozak, David R.
Driscoll, Jefferson I.
Messina, Michael A.
Narpala, Sandeep
Hopp, Christine S.
Cagigi, Alberto
Casazza, Joseph P.
Yamamoto, Takuya
Zhou, Tongqing
Schief, William R.
Crompton, Peter D.
Ledgerwood, Julie E.
Connors, Mark
Gama, Lucio
Kwong, Peter D.
McDermott, Adrian
Mascola, John R.
Koup, Richard A.
author_sort Boswell, Kristin L.
collection PubMed
description The isolation and characterization of neutralizing antibodies from infection and vaccine settings informs future vaccine design, and methodologies that streamline the isolation of antibodies and the generation of B cell clones are of great interest. Retroviral transduction to express Bcl-6 and Bcl-xL and transform primary B cells has been shown to promote long-term B cell survival and antibody secretion in vitro, and can be used to isolate antibodies from memory B cells. However, application of this methodology to B cell subsets from different tissues and B cells from chronically infected individuals has not been well characterized. Here, we characterize Bcl-6/Bcl-xL B cell immortalization across multiple tissue types and B cell subsets in healthy and HIV-1 infected individuals, as well as individuals recovering from malaria. In healthy individuals, naïve and memory B cell subsets from PBMCs and tonsil tissue transformed with similar efficiencies, and displayed similar characteristics with respect to their longevity and immunoglobulin secretion. In HIV-1-viremic individuals or in individuals with recent malaria infections, the exhausted CD27(-)CD21(-) memory B cells transformed with lower efficiency, but the transformed B cells expanded and secreted IgG with similar efficiency. Importantly, we show that this methodology can be used to isolate broadly neutralizing antibodies from HIV-infected individuals. Overall, we demonstrate that Bcl-6/Bcl-xL B cell immortalization can be used to isolate antibodies and generate B cell clones from different B cell populations, albeit with varying efficiencies.
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spelling pubmed-97941412022-12-28 Application of B cell immortalization for the isolation of antibodies and B cell clones from vaccine and infection settings Boswell, Kristin L. Watkins, Timothy A. Cale, Evan M. Samsel, Jakob Andrews, Sarah F. Ambrozak, David R. Driscoll, Jefferson I. Messina, Michael A. Narpala, Sandeep Hopp, Christine S. Cagigi, Alberto Casazza, Joseph P. Yamamoto, Takuya Zhou, Tongqing Schief, William R. Crompton, Peter D. Ledgerwood, Julie E. Connors, Mark Gama, Lucio Kwong, Peter D. McDermott, Adrian Mascola, John R. Koup, Richard A. Front Immunol Immunology The isolation and characterization of neutralizing antibodies from infection and vaccine settings informs future vaccine design, and methodologies that streamline the isolation of antibodies and the generation of B cell clones are of great interest. Retroviral transduction to express Bcl-6 and Bcl-xL and transform primary B cells has been shown to promote long-term B cell survival and antibody secretion in vitro, and can be used to isolate antibodies from memory B cells. However, application of this methodology to B cell subsets from different tissues and B cells from chronically infected individuals has not been well characterized. Here, we characterize Bcl-6/Bcl-xL B cell immortalization across multiple tissue types and B cell subsets in healthy and HIV-1 infected individuals, as well as individuals recovering from malaria. In healthy individuals, naïve and memory B cell subsets from PBMCs and tonsil tissue transformed with similar efficiencies, and displayed similar characteristics with respect to their longevity and immunoglobulin secretion. In HIV-1-viremic individuals or in individuals with recent malaria infections, the exhausted CD27(-)CD21(-) memory B cells transformed with lower efficiency, but the transformed B cells expanded and secreted IgG with similar efficiency. Importantly, we show that this methodology can be used to isolate broadly neutralizing antibodies from HIV-infected individuals. Overall, we demonstrate that Bcl-6/Bcl-xL B cell immortalization can be used to isolate antibodies and generate B cell clones from different B cell populations, albeit with varying efficiencies. Frontiers Media S.A. 2022-12-13 /pmc/articles/PMC9794141/ /pubmed/36582240 http://dx.doi.org/10.3389/fimmu.2022.1087018 Text en Copyright © 2022 Boswell, Watkins, Cale, Samsel, Andrews, Ambrozak, Driscoll, Messina, Narpala, Hopp, Cagigi, Casazza, Yamamoto, Zhou, Schief, Crompton, Ledgerwood, Connors, Gama, Kwong, McDermott, Mascola and Koup 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
Boswell, Kristin L.
Watkins, Timothy A.
Cale, Evan M.
Samsel, Jakob
Andrews, Sarah F.
Ambrozak, David R.
Driscoll, Jefferson I.
Messina, Michael A.
Narpala, Sandeep
Hopp, Christine S.
Cagigi, Alberto
Casazza, Joseph P.
Yamamoto, Takuya
Zhou, Tongqing
Schief, William R.
Crompton, Peter D.
Ledgerwood, Julie E.
Connors, Mark
Gama, Lucio
Kwong, Peter D.
McDermott, Adrian
Mascola, John R.
Koup, Richard A.
Application of B cell immortalization for the isolation of antibodies and B cell clones from vaccine and infection settings
title Application of B cell immortalization for the isolation of antibodies and B cell clones from vaccine and infection settings
title_full Application of B cell immortalization for the isolation of antibodies and B cell clones from vaccine and infection settings
title_fullStr Application of B cell immortalization for the isolation of antibodies and B cell clones from vaccine and infection settings
title_full_unstemmed Application of B cell immortalization for the isolation of antibodies and B cell clones from vaccine and infection settings
title_short Application of B cell immortalization for the isolation of antibodies and B cell clones from vaccine and infection settings
title_sort application of b cell immortalization for the isolation of antibodies and b cell clones from vaccine and infection settings
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9794141/
https://www.ncbi.nlm.nih.gov/pubmed/36582240
http://dx.doi.org/10.3389/fimmu.2022.1087018
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