A humanized CD3ε-knock-in mouse model for pre-clinical testing of anti-human CD3 therapy

Pre-clinical murine models are critical for translating drug candidates from the bench to the bedside. There is interest in better understanding how anti-human CD3 therapy works based on recent longitudinal studies of short-term administration. Although several models have been created in this pursu...

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Autores principales: Crespo, Joel, Koh, Yi Ting, Hu, Ningjie, Moore, Paul A., Bonvini, Ezio, Glasebrook, Andrew L., Martin, Andrea P., Benschop, Robert J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7888618/
https://www.ncbi.nlm.nih.gov/pubmed/33596227
http://dx.doi.org/10.1371/journal.pone.0245917
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author Crespo, Joel
Koh, Yi Ting
Hu, Ningjie
Moore, Paul A.
Bonvini, Ezio
Glasebrook, Andrew L.
Martin, Andrea P.
Benschop, Robert J.
author_facet Crespo, Joel
Koh, Yi Ting
Hu, Ningjie
Moore, Paul A.
Bonvini, Ezio
Glasebrook, Andrew L.
Martin, Andrea P.
Benschop, Robert J.
author_sort Crespo, Joel
collection PubMed
description Pre-clinical murine models are critical for translating drug candidates from the bench to the bedside. There is interest in better understanding how anti-human CD3 therapy works based on recent longitudinal studies of short-term administration. Although several models have been created in this pursuit, each have their own advantages and disadvantages in Type-1 diabetes. In this study, we report a murine genetic knock-in model which expresses both a murine and a humanized-CD3ε-exon, rendering it sensitive to manipulation with anti-human CD3. These huCD3ε(HET) mice are viable and display no gross abnormalities. Specifically, thymocyte development and T cell peripheral homeostasis is unaffected. We tested immune functionality of these mice by immunizing them with T cell-dependent antigens and no differences in antibody titers compared to wild type mice were recorded. Finally, we performed a graft-vs-host disease model that is driven by effector T cell responses and observed a wasting disease upon transfer of huCD3ε(HET) T cells. Our results show a viable humanized CD3 murine model that develops normally, is functionally engaged by anti-human CD3 and can instruct on pre-clinical tests of anti-human CD3 antibodies.
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spelling pubmed-78886182021-02-23 A humanized CD3ε-knock-in mouse model for pre-clinical testing of anti-human CD3 therapy Crespo, Joel Koh, Yi Ting Hu, Ningjie Moore, Paul A. Bonvini, Ezio Glasebrook, Andrew L. Martin, Andrea P. Benschop, Robert J. PLoS One Research Article Pre-clinical murine models are critical for translating drug candidates from the bench to the bedside. There is interest in better understanding how anti-human CD3 therapy works based on recent longitudinal studies of short-term administration. Although several models have been created in this pursuit, each have their own advantages and disadvantages in Type-1 diabetes. In this study, we report a murine genetic knock-in model which expresses both a murine and a humanized-CD3ε-exon, rendering it sensitive to manipulation with anti-human CD3. These huCD3ε(HET) mice are viable and display no gross abnormalities. Specifically, thymocyte development and T cell peripheral homeostasis is unaffected. We tested immune functionality of these mice by immunizing them with T cell-dependent antigens and no differences in antibody titers compared to wild type mice were recorded. Finally, we performed a graft-vs-host disease model that is driven by effector T cell responses and observed a wasting disease upon transfer of huCD3ε(HET) T cells. Our results show a viable humanized CD3 murine model that develops normally, is functionally engaged by anti-human CD3 and can instruct on pre-clinical tests of anti-human CD3 antibodies. Public Library of Science 2021-02-17 /pmc/articles/PMC7888618/ /pubmed/33596227 http://dx.doi.org/10.1371/journal.pone.0245917 Text en © 2021 Crespo et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Crespo, Joel
Koh, Yi Ting
Hu, Ningjie
Moore, Paul A.
Bonvini, Ezio
Glasebrook, Andrew L.
Martin, Andrea P.
Benschop, Robert J.
A humanized CD3ε-knock-in mouse model for pre-clinical testing of anti-human CD3 therapy
title A humanized CD3ε-knock-in mouse model for pre-clinical testing of anti-human CD3 therapy
title_full A humanized CD3ε-knock-in mouse model for pre-clinical testing of anti-human CD3 therapy
title_fullStr A humanized CD3ε-knock-in mouse model for pre-clinical testing of anti-human CD3 therapy
title_full_unstemmed A humanized CD3ε-knock-in mouse model for pre-clinical testing of anti-human CD3 therapy
title_short A humanized CD3ε-knock-in mouse model for pre-clinical testing of anti-human CD3 therapy
title_sort humanized cd3ε-knock-in mouse model for pre-clinical testing of anti-human cd3 therapy
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7888618/
https://www.ncbi.nlm.nih.gov/pubmed/33596227
http://dx.doi.org/10.1371/journal.pone.0245917
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