The establishment of B cell-deficient Igh-J KO mouse model by gene editing and efficacy evaluation

The establishment of B cell-deficient Igh-J KO mouse model by gene editing and efficacy evaluation

•We established a B cell-deficient mouse model by gene editing.•Destroing IghJ genes resulted in mouse B cell depletion but had no effect on overall differentiation and development of other cell types.•B cell-deficient mice can provide functional NK and T cells for tumor immunotherapy.•B cell-defici...

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Veröffentlicht in:International immunopharmacology 2023-03, Vol.116, p.109704-109704, Article 109704
Hauptverfasser: Yu, Xingyan, Li, Tao, Shen, Zhiyuan, Jing, Hongyan, Xie, Xiulong, Zhou, Xiaofei, Shen, Yuelei, Yang, Yi
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Sprache:eng
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Animals
Anti-drug antibodies
Antibodies, Monoclonal - pharmacology
B cell-deficient
B7-H1 Antigen - metabolism
Disease Models, Animal
Gene Editing
Humans
Immunogenicity
Mice
Neoplasms
Preclinical mouse model
Programmed Cell Death 1 Receptor - metabolism
T-Lymphocytes
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container_end_page 109704
container_issue
container_start_page 109704
container_title International immunopharmacology
container_volume 116
creator Yu, Xingyan
Li, Tao
Shen, Zhiyuan
Jing, Hongyan
Xie, Xiulong
Zhou, Xiaofei
Shen, Yuelei
Yang, Yi
description •We established a B cell-deficient mouse model by gene editing.•Destroing IghJ genes resulted in mouse B cell depletion but had no effect on overall differentiation and development of other cell types.•B cell-deficient mice can provide functional NK and T cells for tumor immunotherapy.•B cell-deficient mice were effective in avoiding anti-drug antibodies due to immunogenicity. Over the last few years, immunotherapy has made significant progress in treating various cancers with therapeutic antibodies. However, therapeutic antibodies have been validated for inducing an unintended immune response in human and animal models, which leads to the emergence of anti-drug antibodies (ADAs) and affects their effectiveness and safety. In preclinical research, ADAs production by B cells may accelerate antibody metabolism and result in missing potential candidate molecules. Thus, it is urgent to develop preclinical models that remove only B cells without affecting the function of T and NK cells. Rearrangement of immunoglobulin heavy chain J gene fragment (Igh-J) is the first link in B cell development, and immunotherapies are currently leaning toward combination treatments with PD-1/PD-L1 antibodies, here we created humanized PD-1, PD-L1 and Igh-J knockout (hPD-1/hPD-L1, Igh-J KO) mice and validated by using the reported high immunogenicity drug M7824 (a protein designed to simultaneously block PD-L1 and TGF-β pathways, poorly anti-tumor efficacy in immunocompetent mice). Phenotypic analysis revealed that human PD-1 and PD-L1 were detectable in hPD-1/hPD-L1, Igh-J KO mice, but not mouse IgM and IgD. Igh-J KO depleted B cells while increased the percentage of other immune cell types. Meanwhile, the humanization of PD-1/PD-L1 and Igh-J KO had neither effect on the overall development, differentiation, or distribution of T cell subtypes, nor on the activation of NK and T cells, indicating that mice can be used for T and NK-related immunotherapies. Furthermore, M7824 treatment of these B cell-deficient mice inhibited tumor growth significantly, with higher M7824 analog concentrations and lower ADA-positive rates. These findings demonstrate that Igh-J KO mice are an effective and stable preclinical model for testing drugs based on T and NK cells with high immunogenicity in vivo.
doi_str_mv 10.1016/j.intimp.2023.109704
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Over the last few years, immunotherapy has made significant progress in treating various cancers with therapeutic antibodies. However, therapeutic antibodies have been validated for inducing an unintended immune response in human and animal models, which leads to the emergence of anti-drug antibodies (ADAs) and affects their effectiveness and safety. In preclinical research, ADAs production by B cells may accelerate antibody metabolism and result in missing potential candidate molecules. Thus, it is urgent to develop preclinical models that remove only B cells without affecting the function of T and NK cells. Rearrangement of immunoglobulin heavy chain J gene fragment (Igh-J) is the first link in B cell development, and immunotherapies are currently leaning toward combination treatments with PD-1/PD-L1 antibodies, here we created humanized PD-1, PD-L1 and Igh-J knockout (hPD-1/hPD-L1, Igh-J KO) mice and validated by using the reported high immunogenicity drug M7824 (a protein designed to simultaneously block PD-L1 and TGF-β pathways, poorly anti-tumor efficacy in immunocompetent mice). Phenotypic analysis revealed that human PD-1 and PD-L1 were detectable in hPD-1/hPD-L1, Igh-J KO mice, but not mouse IgM and IgD. Igh-J KO depleted B cells while increased the percentage of other immune cell types. Meanwhile, the humanization of PD-1/PD-L1 and Igh-J KO had neither effect on the overall development, differentiation, or distribution of T cell subtypes, nor on the activation of NK and T cells, indicating that mice can be used for T and NK-related immunotherapies. Furthermore, M7824 treatment of these B cell-deficient mice inhibited tumor growth significantly, with higher M7824 analog concentrations and lower ADA-positive rates. 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Over the last few years, immunotherapy has made significant progress in treating various cancers with therapeutic antibodies. However, therapeutic antibodies have been validated for inducing an unintended immune response in human and animal models, which leads to the emergence of anti-drug antibodies (ADAs) and affects their effectiveness and safety. In preclinical research, ADAs production by B cells may accelerate antibody metabolism and result in missing potential candidate molecules. Thus, it is urgent to develop preclinical models that remove only B cells without affecting the function of T and NK cells. Rearrangement of immunoglobulin heavy chain J gene fragment (Igh-J) is the first link in B cell development, and immunotherapies are currently leaning toward combination treatments with PD-1/PD-L1 antibodies, here we created humanized PD-1, PD-L1 and Igh-J knockout (hPD-1/hPD-L1, Igh-J KO) mice and validated by using the reported high immunogenicity drug M7824 (a protein designed to simultaneously block PD-L1 and TGF-β pathways, poorly anti-tumor efficacy in immunocompetent mice). Phenotypic analysis revealed that human PD-1 and PD-L1 were detectable in hPD-1/hPD-L1, Igh-J KO mice, but not mouse IgM and IgD. Igh-J KO depleted B cells while increased the percentage of other immune cell types. Meanwhile, the humanization of PD-1/PD-L1 and Igh-J KO had neither effect on the overall development, differentiation, or distribution of T cell subtypes, nor on the activation of NK and T cells, indicating that mice can be used for T and NK-related immunotherapies. Furthermore, M7824 treatment of these B cell-deficient mice inhibited tumor growth significantly, with higher M7824 analog concentrations and lower ADA-positive rates. These findings demonstrate that Igh-J KO mice are an effective and stable preclinical model for testing drugs based on T and NK cells with high immunogenicity in vivo.</description><subject>Animals</subject><subject>Anti-drug antibodies</subject><subject>Antibodies, Monoclonal - pharmacology</subject><subject>B cell-deficient</subject><subject>B7-H1 Antigen - metabolism</subject><subject>Disease Models, Animal</subject><subject>Gene Editing</subject><subject>Humans</subject><subject>Immunogenicity</subject><subject>Mice</subject><subject>Neoplasms</subject><subject>Preclinical mouse model</subject><subject>Programmed Cell Death 1 Receptor - metabolism</subject><subject>T-Lymphocytes</subject><issn>1567-5769</issn><issn>1878-1705</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2023</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNp9kEtPAjEUhRujEUT_gTFduhls59XpxkSJD5SEDa6bPm6hZB44HUj493Yy6NJN25yc03vPh9AtJVNKaP6wnbq6c9VuGpM4CRJnJD1DY1qwIqKMZOfhneUsyljOR-jK-y0hQU_pJRoleV7wImVjpFYbwOA7qUrnNxXUHW4sfsYayjIyYJ12vTZfb6IP_LnEVbP3EE4DJVZHvIY6xI3rXL3GsjYYbIhIfcRwkOVedq6pr9GFlaWHm9M9QV-vL6vZe7RYvs1nT4tIJ5R2EedWm9iY1EqprJJE0oRkylIAKnNuYqUk8LgwBApjKeNJxiRVVMVKsozoZILuh393bfO9D51E5XzfQ9YQthZxAJEEZ5EGazpYddt434IVu9ZVsj0KSkRPV2zFQFf0dMVAN8TuThP2qgLzF_rFGQyPgwFCz4ODVvienw6EWtCdMI37f8IPhUCOSw</recordid><startdate>202303</startdate><enddate>202303</enddate><creator>Yu, Xingyan</creator><creator>Li, Tao</creator><creator>Shen, Zhiyuan</creator><creator>Jing, Hongyan</creator><creator>Xie, Xiulong</creator><creator>Zhou, Xiaofei</creator><creator>Shen, Yuelei</creator><creator>Yang, Yi</creator><general>Elsevier B.V</general><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope></search><sort><creationdate>202303</creationdate><title>The establishment of B cell-deficient Igh-J KO mouse model by gene editing and efficacy evaluation</title><author>Yu, Xingyan ; Li, Tao ; Shen, Zhiyuan ; Jing, Hongyan ; Xie, Xiulong ; Zhou, Xiaofei ; Shen, Yuelei ; Yang, Yi</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-c311t-99fcd2dd4faabfba0a1305bf1ee1a69d2bbae928d0e8df179357a1b1b2ba750c3</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2023</creationdate><topic>Animals</topic><topic>Anti-drug antibodies</topic><topic>Antibodies, Monoclonal - pharmacology</topic><topic>B cell-deficient</topic><topic>B7-H1 Antigen - metabolism</topic><topic>Disease Models, Animal</topic><topic>Gene Editing</topic><topic>Humans</topic><topic>Immunogenicity</topic><topic>Mice</topic><topic>Neoplasms</topic><topic>Preclinical mouse model</topic><topic>Programmed Cell Death 1 Receptor - metabolism</topic><topic>T-Lymphocytes</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Yu, Xingyan</creatorcontrib><creatorcontrib>Li, Tao</creatorcontrib><creatorcontrib>Shen, Zhiyuan</creatorcontrib><creatorcontrib>Jing, Hongyan</creatorcontrib><creatorcontrib>Xie, Xiulong</creatorcontrib><creatorcontrib>Zhou, Xiaofei</creatorcontrib><creatorcontrib>Shen, Yuelei</creatorcontrib><creatorcontrib>Yang, Yi</creatorcontrib><collection>Medline</collection><collection>MEDLINE</collection><collection>MEDLINE (Ovid)</collection><collection>MEDLINE</collection><collection>MEDLINE</collection><collection>PubMed</collection><collection>CrossRef</collection><collection>MEDLINE - Academic</collection><jtitle>International immunopharmacology</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Yu, Xingyan</au><au>Li, Tao</au><au>Shen, Zhiyuan</au><au>Jing, Hongyan</au><au>Xie, Xiulong</au><au>Zhou, Xiaofei</au><au>Shen, Yuelei</au><au>Yang, Yi</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>The establishment of B cell-deficient Igh-J KO mouse model by gene editing and efficacy evaluation</atitle><jtitle>International immunopharmacology</jtitle><addtitle>Int Immunopharmacol</addtitle><date>2023-03</date><risdate>2023</risdate><volume>116</volume><spage>109704</spage><epage>109704</epage><pages>109704-109704</pages><artnum>109704</artnum><issn>1567-5769</issn><eissn>1878-1705</eissn><abstract>•We established a B cell-deficient mouse model by gene editing.•Destroing IghJ genes resulted in mouse B cell depletion but had no effect on overall differentiation and development of other cell types.•B cell-deficient mice can provide functional NK and T cells for tumor immunotherapy.•B cell-deficient mice were effective in avoiding anti-drug antibodies due to immunogenicity. Over the last few years, immunotherapy has made significant progress in treating various cancers with therapeutic antibodies. However, therapeutic antibodies have been validated for inducing an unintended immune response in human and animal models, which leads to the emergence of anti-drug antibodies (ADAs) and affects their effectiveness and safety. In preclinical research, ADAs production by B cells may accelerate antibody metabolism and result in missing potential candidate molecules. Thus, it is urgent to develop preclinical models that remove only B cells without affecting the function of T and NK cells. Rearrangement of immunoglobulin heavy chain J gene fragment (Igh-J) is the first link in B cell development, and immunotherapies are currently leaning toward combination treatments with PD-1/PD-L1 antibodies, here we created humanized PD-1, PD-L1 and Igh-J knockout (hPD-1/hPD-L1, Igh-J KO) mice and validated by using the reported high immunogenicity drug M7824 (a protein designed to simultaneously block PD-L1 and TGF-β pathways, poorly anti-tumor efficacy in immunocompetent mice). Phenotypic analysis revealed that human PD-1 and PD-L1 were detectable in hPD-1/hPD-L1, Igh-J KO mice, but not mouse IgM and IgD. Igh-J KO depleted B cells while increased the percentage of other immune cell types. Meanwhile, the humanization of PD-1/PD-L1 and Igh-J KO had neither effect on the overall development, differentiation, or distribution of T cell subtypes, nor on the activation of NK and T cells, indicating that mice can be used for T and NK-related immunotherapies. Furthermore, M7824 treatment of these B cell-deficient mice inhibited tumor growth significantly, with higher M7824 analog concentrations and lower ADA-positive rates. These findings demonstrate that Igh-J KO mice are an effective and stable preclinical model for testing drugs based on T and NK cells with high immunogenicity in vivo.</abstract><cop>Netherlands</cop><pub>Elsevier B.V</pub><pmid>36689847</pmid><doi>10.1016/j.intimp.2023.109704</doi><tpages>1</tpages></addata></record>
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subjects Animals
Anti-drug antibodies
Antibodies, Monoclonal - pharmacology
B cell-deficient
B7-H1 Antigen - metabolism
Disease Models, Animal
Gene Editing
Humans
Immunogenicity
Mice
Neoplasms
Preclinical mouse model
Programmed Cell Death 1 Receptor - metabolism
T-Lymphocytes
title The establishment of B cell-deficient Igh-J KO mouse model by gene editing and efficacy evaluation
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