Creation of an immunodeficient HLA-transgenic mouse (HUMAMICE) and functional validation of human immunity after transfer of HLA-matched human cells

Research on human immunology has been hindered by the lack of optimal small animal models, given that the protective immune responses of human and non-human species show significant differences. However, due to ethical constraints[1] and the high cost of clinical trials, it is urgent to improve the...

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Autores principales: Zeng, Yang, Liu, Bingrun, Rubio, Marie-Thérèse, Wang, Xinyue, Ojcius, David M., Tang, Ruoping, Durrbach, Antoine, Ru, Zhitao, Zhou, Yusen, Lone, Yu-Chun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5388326/
https://www.ncbi.nlm.nih.gov/pubmed/28399128
http://dx.doi.org/10.1371/journal.pone.0173754
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author Zeng, Yang
Liu, Bingrun
Rubio, Marie-Thérèse
Wang, Xinyue
Ojcius, David M.
Tang, Ruoping
Durrbach, Antoine
Ru, Zhitao
Zhou, Yusen
Lone, Yu-Chun
author_facet Zeng, Yang
Liu, Bingrun
Rubio, Marie-Thérèse
Wang, Xinyue
Ojcius, David M.
Tang, Ruoping
Durrbach, Antoine
Ru, Zhitao
Zhou, Yusen
Lone, Yu-Chun
author_sort Zeng, Yang
collection PubMed
description Research on human immunology has been hindered by the lack of optimal small animal models, given that the protective immune responses of human and non-human species show significant differences. However, due to ethical constraints[1] and the high cost of clinical trials, it is urgent to improve the current animal models that can mimic faithfully human physiology, particularly the human immune system (HIS). HIS mice had been generated recently by engrafting human hematopoietic stem cells (hHSCs) or human peripheral mononuclear cells (hPBMCs) into highly immuno-deficient mice such as NSG, NOG or NRG mice. However, a major experimental drawback for studies using these models is the rapid onset of Graft-versus-Host Disease (GvHD). In the present study, we overcome this limitation by generating new immuno-deficient mice named "HUMAMICE" (HLA-A2(+/+)/DR1(+/+)/H-2-β(2)m(-/-)/IAβ(-/-)/Rag2(-/-)/IL2rγ(-/-)/Perf(-/-) mice), which expressed human HLA molecules instead of mouse MHC molecules (H-2), and whose immuno-deficient status was reversed by transferring functional HLA-matched PBMCs thus producing mice with an immuno-competent status with a functional human immune system. We showed that in this HLA-matched context, the hPBMC-transfer led to high lymphocytes engraftment rates without GvHD over three months in this novel mouse model. Furthermore, to evaluate the utility of the hPBMC-HUMAMICE, we immunized them with commercial vaccine of Hepatitis B virus (HBsAg, Hepvac@) which resulted in robust and reproducible production of high levels of HBsAg-specific antibodies, implying that both transferred T and B lymphocytes were functional in HUMAMICE. These responses are comparable to those observed in human clinical trials with this identical vaccine. In conclusion, these findings indicated that the HLA-matched-hPBMC-HUMAMICE represents a promising model for dissecting human immune responses in various human diseases, including infectious diseases, cancers and tumors, and to facilitate the development of novel vaccines and cellular therapies.
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spelling pubmed-53883262017-05-03 Creation of an immunodeficient HLA-transgenic mouse (HUMAMICE) and functional validation of human immunity after transfer of HLA-matched human cells Zeng, Yang Liu, Bingrun Rubio, Marie-Thérèse Wang, Xinyue Ojcius, David M. Tang, Ruoping Durrbach, Antoine Ru, Zhitao Zhou, Yusen Lone, Yu-Chun PLoS One Research Article Research on human immunology has been hindered by the lack of optimal small animal models, given that the protective immune responses of human and non-human species show significant differences. However, due to ethical constraints[1] and the high cost of clinical trials, it is urgent to improve the current animal models that can mimic faithfully human physiology, particularly the human immune system (HIS). HIS mice had been generated recently by engrafting human hematopoietic stem cells (hHSCs) or human peripheral mononuclear cells (hPBMCs) into highly immuno-deficient mice such as NSG, NOG or NRG mice. However, a major experimental drawback for studies using these models is the rapid onset of Graft-versus-Host Disease (GvHD). In the present study, we overcome this limitation by generating new immuno-deficient mice named "HUMAMICE" (HLA-A2(+/+)/DR1(+/+)/H-2-β(2)m(-/-)/IAβ(-/-)/Rag2(-/-)/IL2rγ(-/-)/Perf(-/-) mice), which expressed human HLA molecules instead of mouse MHC molecules (H-2), and whose immuno-deficient status was reversed by transferring functional HLA-matched PBMCs thus producing mice with an immuno-competent status with a functional human immune system. We showed that in this HLA-matched context, the hPBMC-transfer led to high lymphocytes engraftment rates without GvHD over three months in this novel mouse model. Furthermore, to evaluate the utility of the hPBMC-HUMAMICE, we immunized them with commercial vaccine of Hepatitis B virus (HBsAg, Hepvac@) which resulted in robust and reproducible production of high levels of HBsAg-specific antibodies, implying that both transferred T and B lymphocytes were functional in HUMAMICE. These responses are comparable to those observed in human clinical trials with this identical vaccine. In conclusion, these findings indicated that the HLA-matched-hPBMC-HUMAMICE represents a promising model for dissecting human immune responses in various human diseases, including infectious diseases, cancers and tumors, and to facilitate the development of novel vaccines and cellular therapies. Public Library of Science 2017-04-11 /pmc/articles/PMC5388326/ /pubmed/28399128 http://dx.doi.org/10.1371/journal.pone.0173754 Text en © 2017 Zeng 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
Zeng, Yang
Liu, Bingrun
Rubio, Marie-Thérèse
Wang, Xinyue
Ojcius, David M.
Tang, Ruoping
Durrbach, Antoine
Ru, Zhitao
Zhou, Yusen
Lone, Yu-Chun
Creation of an immunodeficient HLA-transgenic mouse (HUMAMICE) and functional validation of human immunity after transfer of HLA-matched human cells
title Creation of an immunodeficient HLA-transgenic mouse (HUMAMICE) and functional validation of human immunity after transfer of HLA-matched human cells
title_full Creation of an immunodeficient HLA-transgenic mouse (HUMAMICE) and functional validation of human immunity after transfer of HLA-matched human cells
title_fullStr Creation of an immunodeficient HLA-transgenic mouse (HUMAMICE) and functional validation of human immunity after transfer of HLA-matched human cells
title_full_unstemmed Creation of an immunodeficient HLA-transgenic mouse (HUMAMICE) and functional validation of human immunity after transfer of HLA-matched human cells
title_short Creation of an immunodeficient HLA-transgenic mouse (HUMAMICE) and functional validation of human immunity after transfer of HLA-matched human cells
title_sort creation of an immunodeficient hla-transgenic mouse (humamice) and functional validation of human immunity after transfer of hla-matched human cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5388326/
https://www.ncbi.nlm.nih.gov/pubmed/28399128
http://dx.doi.org/10.1371/journal.pone.0173754
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