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Rabbits transgenic for human IgG genes recapitulating rabbit B-cell biology to generate human antibodies of high specificity and affinity

Transgenic animals incorporating human antibody genes are extremely attractive for drug development because they obviate subsequent antibody humanization procedures required for therapeutic translation. Transgenic platforms have previously been established using mice, but also more recently rats, ch...

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Autores principales: Ros, Francesca, Offner, Sonja, Klostermann, Stefan, Thorey, Irmgard, Niersbach, Helmut, Breuer, Sebastian, Zarnt, Grit, Lorenz, Stefan, Puels, Juergen, Siewe, Basile, Schueler, Nicole, Dragicevic, Tajana, Ostler, Dominique, Hansen-Wester, Imke, Lifke, Valeria, Kaluza, Brigitte, Kaluza, Klaus, van Schooten, Wim, Buelow, Roland, Tissot, Alain C, Platzer, Josef
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Taylor & Francis 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7780963/
https://www.ncbi.nlm.nih.gov/pubmed/33228444
http://dx.doi.org/10.1080/19420862.2020.1846900
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author Ros, Francesca
Offner, Sonja
Klostermann, Stefan
Thorey, Irmgard
Niersbach, Helmut
Breuer, Sebastian
Zarnt, Grit
Lorenz, Stefan
Puels, Juergen
Siewe, Basile
Schueler, Nicole
Dragicevic, Tajana
Ostler, Dominique
Hansen-Wester, Imke
Lifke, Valeria
Kaluza, Brigitte
Kaluza, Klaus
van Schooten, Wim
Buelow, Roland
Tissot, Alain C
Platzer, Josef
author_facet Ros, Francesca
Offner, Sonja
Klostermann, Stefan
Thorey, Irmgard
Niersbach, Helmut
Breuer, Sebastian
Zarnt, Grit
Lorenz, Stefan
Puels, Juergen
Siewe, Basile
Schueler, Nicole
Dragicevic, Tajana
Ostler, Dominique
Hansen-Wester, Imke
Lifke, Valeria
Kaluza, Brigitte
Kaluza, Klaus
van Schooten, Wim
Buelow, Roland
Tissot, Alain C
Platzer, Josef
author_sort Ros, Francesca
collection PubMed
description Transgenic animals incorporating human antibody genes are extremely attractive for drug development because they obviate subsequent antibody humanization procedures required for therapeutic translation. Transgenic platforms have previously been established using mice, but also more recently rats, chickens, and cows and are now in abundant use for drug development. However, rabbit-based antibody generation, with a strong track record for specificity and affinity, is able to include gene conversion mediated sequence diversification, thereby enhancing binder maturation and improving the variance/selection of output antibodies in a different way than in rodents. Since it additionally frequently permits good binder generation against antigens that are only weakly immunogenic in other organisms, it is a highly interesting species for therapeutic antibody generation. We report here on the generation, utilization, and analysis of the first transgenic rabbit strain for human antibody production. Through the knockout of endogenous IgM genes and the introduction of human immunoglobulin sequences, this rabbit strain has been engineered to generate a highly diverse human IgG antibody repertoire. We further incorporated human CD79a/b and Bcl2 (B-cell lymphoma 2) genes, which enhance B-cell receptor expression and B-cell survival. Following immunization against the angiogenic factor BMP9 (Bone Morphogenetic Proteins 9), we were able to isolate a set of exquisitely affine and specific neutralizing antibodies from these rabbits. Sequence analysis of these binders revealed that both somatic hypermutation and gene conversion are fully operational in this strain, without compromising the very high degree of humanness. This powerful new transgenic strategy will allow further expansion of the use of endogenous immune mechanisms in drug development.
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spelling pubmed-77809632021-01-13 Rabbits transgenic for human IgG genes recapitulating rabbit B-cell biology to generate human antibodies of high specificity and affinity Ros, Francesca Offner, Sonja Klostermann, Stefan Thorey, Irmgard Niersbach, Helmut Breuer, Sebastian Zarnt, Grit Lorenz, Stefan Puels, Juergen Siewe, Basile Schueler, Nicole Dragicevic, Tajana Ostler, Dominique Hansen-Wester, Imke Lifke, Valeria Kaluza, Brigitte Kaluza, Klaus van Schooten, Wim Buelow, Roland Tissot, Alain C Platzer, Josef MAbs Report Transgenic animals incorporating human antibody genes are extremely attractive for drug development because they obviate subsequent antibody humanization procedures required for therapeutic translation. Transgenic platforms have previously been established using mice, but also more recently rats, chickens, and cows and are now in abundant use for drug development. However, rabbit-based antibody generation, with a strong track record for specificity and affinity, is able to include gene conversion mediated sequence diversification, thereby enhancing binder maturation and improving the variance/selection of output antibodies in a different way than in rodents. Since it additionally frequently permits good binder generation against antigens that are only weakly immunogenic in other organisms, it is a highly interesting species for therapeutic antibody generation. We report here on the generation, utilization, and analysis of the first transgenic rabbit strain for human antibody production. Through the knockout of endogenous IgM genes and the introduction of human immunoglobulin sequences, this rabbit strain has been engineered to generate a highly diverse human IgG antibody repertoire. We further incorporated human CD79a/b and Bcl2 (B-cell lymphoma 2) genes, which enhance B-cell receptor expression and B-cell survival. Following immunization against the angiogenic factor BMP9 (Bone Morphogenetic Proteins 9), we were able to isolate a set of exquisitely affine and specific neutralizing antibodies from these rabbits. Sequence analysis of these binders revealed that both somatic hypermutation and gene conversion are fully operational in this strain, without compromising the very high degree of humanness. This powerful new transgenic strategy will allow further expansion of the use of endogenous immune mechanisms in drug development. Taylor & Francis 2020-11-24 /pmc/articles/PMC7780963/ /pubmed/33228444 http://dx.doi.org/10.1080/19420862.2020.1846900 Text en © 2020 Taylor & Francis Group, LLC https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial License (http://creativecommons.org/licenses/by-nc/4.0/ (https://creativecommons.org/licenses/by-nc/4.0/) ), which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Report
Ros, Francesca
Offner, Sonja
Klostermann, Stefan
Thorey, Irmgard
Niersbach, Helmut
Breuer, Sebastian
Zarnt, Grit
Lorenz, Stefan
Puels, Juergen
Siewe, Basile
Schueler, Nicole
Dragicevic, Tajana
Ostler, Dominique
Hansen-Wester, Imke
Lifke, Valeria
Kaluza, Brigitte
Kaluza, Klaus
van Schooten, Wim
Buelow, Roland
Tissot, Alain C
Platzer, Josef
Rabbits transgenic for human IgG genes recapitulating rabbit B-cell biology to generate human antibodies of high specificity and affinity
title Rabbits transgenic for human IgG genes recapitulating rabbit B-cell biology to generate human antibodies of high specificity and affinity
title_full Rabbits transgenic for human IgG genes recapitulating rabbit B-cell biology to generate human antibodies of high specificity and affinity
title_fullStr Rabbits transgenic for human IgG genes recapitulating rabbit B-cell biology to generate human antibodies of high specificity and affinity
title_full_unstemmed Rabbits transgenic for human IgG genes recapitulating rabbit B-cell biology to generate human antibodies of high specificity and affinity
title_short Rabbits transgenic for human IgG genes recapitulating rabbit B-cell biology to generate human antibodies of high specificity and affinity
title_sort rabbits transgenic for human igg genes recapitulating rabbit b-cell biology to generate human antibodies of high specificity and affinity
topic Report
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7780963/
https://www.ncbi.nlm.nih.gov/pubmed/33228444
http://dx.doi.org/10.1080/19420862.2020.1846900
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