Multiplexed CRISPR/CAS9‐mediated engineering of pre‐clinical mouse models bearing native human B cell receptors

B‐cell receptor (BCR) knock‐in (KI) mouse models play an important role in vaccine development and fundamental immunological studies. However, the time required to generate them poses a bottleneck. Here we report a one‐step CRISPR/Cas9 KI methodology to combine the insertion of human germline immuno...

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Autores principales: Wang, Xuesong, Ray, Rashmi, Kratochvil, Sven, Melzi, Eleonora, Lin, Ying‐Cing, Giguere, Sophie, Xu, Liling, Warner, John, Cheon, Diane, Liguori, Alessia, Groschel, Bettina, Phelps, Nicole, Adachi, Yumiko, Tingle, Ryan, Wu, Lin, Crotty, Shane, Kirsch, Kathrin H, Nair, Usha, Schief, William R, Batista, Facundo D
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2020
Materias:
Resources
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7809789/
https://www.ncbi.nlm.nih.gov/pubmed/33258500
http://dx.doi.org/10.15252/embj.2020105926
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author Wang, Xuesong
Ray, Rashmi
Kratochvil, Sven
Melzi, Eleonora
Lin, Ying‐Cing
Giguere, Sophie
Xu, Liling
Warner, John
Cheon, Diane
Liguori, Alessia
Groschel, Bettina
Phelps, Nicole
Adachi, Yumiko
Tingle, Ryan
Wu, Lin
Crotty, Shane
Kirsch, Kathrin H
Nair, Usha
Schief, William R
Batista, Facundo D
author_facet Wang, Xuesong
Ray, Rashmi
Kratochvil, Sven
Melzi, Eleonora
Lin, Ying‐Cing
Giguere, Sophie
Xu, Liling
Warner, John
Cheon, Diane
Liguori, Alessia
Groschel, Bettina
Phelps, Nicole
Adachi, Yumiko
Tingle, Ryan
Wu, Lin
Crotty, Shane
Kirsch, Kathrin H
Nair, Usha
Schief, William R
Batista, Facundo D
author_sort Wang, Xuesong
collection PubMed
description B‐cell receptor (BCR) knock‐in (KI) mouse models play an important role in vaccine development and fundamental immunological studies. However, the time required to generate them poses a bottleneck. Here we report a one‐step CRISPR/Cas9 KI methodology to combine the insertion of human germline immunoglobulin heavy and light chains at their endogenous loci in mice. We validate this technology with the rapid generation of three BCR KI lines expressing native human precursors, instead of computationally inferred germline sequences, to HIV broadly neutralizing antibodies. We demonstrate that B cells from these mice are fully functional: upon transfer to congenic, wild type mice at controlled frequencies, such B cells can be primed by eOD‐GT8 60mer, a germline‐targeting immunogen currently in clinical trials, recruited to germinal centers, secrete class‐switched antibodies, undergo somatic hypermutation, and differentiate into memory B cells. KI mice expressing functional human BCRs promise to accelerate the development of vaccines for HIV and other infectious diseases.
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spelling pubmed-78097892021-01-27 Multiplexed CRISPR/CAS9‐mediated engineering of pre‐clinical mouse models bearing native human B cell receptors Wang, Xuesong Ray, Rashmi Kratochvil, Sven Melzi, Eleonora Lin, Ying‐Cing Giguere, Sophie Xu, Liling Warner, John Cheon, Diane Liguori, Alessia Groschel, Bettina Phelps, Nicole Adachi, Yumiko Tingle, Ryan Wu, Lin Crotty, Shane Kirsch, Kathrin H Nair, Usha Schief, William R Batista, Facundo D EMBO J Resources B‐cell receptor (BCR) knock‐in (KI) mouse models play an important role in vaccine development and fundamental immunological studies. However, the time required to generate them poses a bottleneck. Here we report a one‐step CRISPR/Cas9 KI methodology to combine the insertion of human germline immunoglobulin heavy and light chains at their endogenous loci in mice. We validate this technology with the rapid generation of three BCR KI lines expressing native human precursors, instead of computationally inferred germline sequences, to HIV broadly neutralizing antibodies. We demonstrate that B cells from these mice are fully functional: upon transfer to congenic, wild type mice at controlled frequencies, such B cells can be primed by eOD‐GT8 60mer, a germline‐targeting immunogen currently in clinical trials, recruited to germinal centers, secrete class‐switched antibodies, undergo somatic hypermutation, and differentiate into memory B cells. KI mice expressing functional human BCRs promise to accelerate the development of vaccines for HIV and other infectious diseases. John Wiley and Sons Inc. 2020-12-01 2021-01-15 /pmc/articles/PMC7809789/ /pubmed/33258500 http://dx.doi.org/10.15252/embj.2020105926 Text en © 2020 The Authors. Published under the terms of the CC BY 4.0 license This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Resources
Wang, Xuesong
Ray, Rashmi
Kratochvil, Sven
Melzi, Eleonora
Lin, Ying‐Cing
Giguere, Sophie
Xu, Liling
Warner, John
Cheon, Diane
Liguori, Alessia
Groschel, Bettina
Phelps, Nicole
Adachi, Yumiko
Tingle, Ryan
Wu, Lin
Crotty, Shane
Kirsch, Kathrin H
Nair, Usha
Schief, William R
Batista, Facundo D
Multiplexed CRISPR/CAS9‐mediated engineering of pre‐clinical mouse models bearing native human B cell receptors
title Multiplexed CRISPR/CAS9‐mediated engineering of pre‐clinical mouse models bearing native human B cell receptors
title_full Multiplexed CRISPR/CAS9‐mediated engineering of pre‐clinical mouse models bearing native human B cell receptors
title_fullStr Multiplexed CRISPR/CAS9‐mediated engineering of pre‐clinical mouse models bearing native human B cell receptors
title_full_unstemmed Multiplexed CRISPR/CAS9‐mediated engineering of pre‐clinical mouse models bearing native human B cell receptors
title_short Multiplexed CRISPR/CAS9‐mediated engineering of pre‐clinical mouse models bearing native human B cell receptors
title_sort multiplexed crispr/cas9‐mediated engineering of pre‐clinical mouse models bearing native human b cell receptors
topic Resources
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7809789/
https://www.ncbi.nlm.nih.gov/pubmed/33258500
http://dx.doi.org/10.15252/embj.2020105926
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