Synergistic effect of glutathione and IgG4 in immune evasion and the implication for cancer immunotherapy()

BACKGROUND: We recently reported a novel IgG4-centered immune evasion mechanism in cancer, and this was achieved mostly through the Fc-Fc reaction of increased IgG4 to cancer-bound IgG in cancer microenvironment. The mechanism was suggested to be related to cancer hyperprogressive disease (HPD) whic...

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Autores principales: Zhang, Weifeng, Quan, Yan, Ma, Xiaonan, Zeng, Liting, Li, Jirui, Chen, Shuqi, Su, Meng, Hong, Liangli, Li, Penghao, Wang, Hui, Xu, Qian, Zhao, Chanyuan, Zhu, Xiaoqing, Geng, Yiqun, Yan, Xiaomiao, Fang, Zheng, Chen, Muwang, Tian, Dongping, Su, Min, Chen, Xueling, Gu, Jiang
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2023
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9868885/
https://www.ncbi.nlm.nih.gov/pubmed/36681047
http://dx.doi.org/10.1016/j.redox.2023.102608
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author Zhang, Weifeng
Quan, Yan
Ma, Xiaonan
Zeng, Liting
Li, Jirui
Chen, Shuqi
Su, Meng
Hong, Liangli
Li, Penghao
Wang, Hui
Xu, Qian
Zhao, Chanyuan
Zhu, Xiaoqing
Geng, Yiqun
Yan, Xiaomiao
Fang, Zheng
Chen, Muwang
Tian, Dongping
Su, Min
Chen, Xueling
Gu, Jiang
author_facet Zhang, Weifeng
Quan, Yan
Ma, Xiaonan
Zeng, Liting
Li, Jirui
Chen, Shuqi
Su, Meng
Hong, Liangli
Li, Penghao
Wang, Hui
Xu, Qian
Zhao, Chanyuan
Zhu, Xiaoqing
Geng, Yiqun
Yan, Xiaomiao
Fang, Zheng
Chen, Muwang
Tian, Dongping
Su, Min
Chen, Xueling
Gu, Jiang
author_sort Zhang, Weifeng
collection PubMed
description BACKGROUND: We recently reported a novel IgG4-centered immune evasion mechanism in cancer, and this was achieved mostly through the Fc-Fc reaction of increased IgG4 to cancer-bound IgG in cancer microenvironment. The mechanism was suggested to be related to cancer hyperprogressive disease (HPD) which is a side-effect often associated to IgG4 subtype PD-1 antibody immunotherapy. HPD was reported to occur in cancers with certain mutated genes including KRAS and such mutations are often associated to glutathione (GSH) synthesis. Therefore, we hypothesize that IgG4 and GSH may play a synergistic role in local immunosuppression of cancer. METHODS: Quantitatively analyzed the distribution and abundance of GSH and IgG4 in human cancer samples with ELISA and immunohistochemistry. The interactions between GSH and IgG4 were examined with Electrophoresis and Western Blot. The synergistic effects of the two on classic immune responses were investigated in vitro. The combined effects were also tested in a lung cancer model and a skin graft model in mice. RESULTS: We detected significant increases of both GSH and IgG4 in the microenvironment of lung cancer, esophageal cancer, and colon cancer tissues. GSH disrupted the disulfide bond of IgG4 heavy chain and enhanced IgG4’s ability of Fc-Fc reaction to immobilized IgG subtypes. Combined administration of IgG4 and GSH augmented the inhibitory effect of IgG4 on the classic ADCC, ADCP, and CDC reactions. Local administration of IgG4/GSH achieved the most obvious effect of accelerating cancer growth in the mouse lung cancer model. The same combination prolonged the survival of skin grafts between two different strains of mouse. In both models, immune cells and several cytokines were found to shift to the state of immune tolerance. CONCLUSION: Combined application of GSH and IgG4 can promote tumor growth and protect skin graft. The mechanism may be achieved through the effect of the Fc-Fc reaction between IgG4 and other tissue-bound IgG subtypes resulting in local immunosuppression. This reaction was facilitated by increased GSH to dissociate the two heavy chains of IgG4 Fc fragment at its disulfide bonds. Our findings unveiled the interaction between the redox system and the immune systems in cancer microenvironment. It offers a sensible explanation for HPD and provides new possibilities for manipulating this mechanism for cancer immunotherapy.
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spelling pubmed-98688852023-01-24 Synergistic effect of glutathione and IgG4 in immune evasion and the implication for cancer immunotherapy() Zhang, Weifeng Quan, Yan Ma, Xiaonan Zeng, Liting Li, Jirui Chen, Shuqi Su, Meng Hong, Liangli Li, Penghao Wang, Hui Xu, Qian Zhao, Chanyuan Zhu, Xiaoqing Geng, Yiqun Yan, Xiaomiao Fang, Zheng Chen, Muwang Tian, Dongping Su, Min Chen, Xueling Gu, Jiang Redox Biol Research Paper BACKGROUND: We recently reported a novel IgG4-centered immune evasion mechanism in cancer, and this was achieved mostly through the Fc-Fc reaction of increased IgG4 to cancer-bound IgG in cancer microenvironment. The mechanism was suggested to be related to cancer hyperprogressive disease (HPD) which is a side-effect often associated to IgG4 subtype PD-1 antibody immunotherapy. HPD was reported to occur in cancers with certain mutated genes including KRAS and such mutations are often associated to glutathione (GSH) synthesis. Therefore, we hypothesize that IgG4 and GSH may play a synergistic role in local immunosuppression of cancer. METHODS: Quantitatively analyzed the distribution and abundance of GSH and IgG4 in human cancer samples with ELISA and immunohistochemistry. The interactions between GSH and IgG4 were examined with Electrophoresis and Western Blot. The synergistic effects of the two on classic immune responses were investigated in vitro. The combined effects were also tested in a lung cancer model and a skin graft model in mice. RESULTS: We detected significant increases of both GSH and IgG4 in the microenvironment of lung cancer, esophageal cancer, and colon cancer tissues. GSH disrupted the disulfide bond of IgG4 heavy chain and enhanced IgG4’s ability of Fc-Fc reaction to immobilized IgG subtypes. Combined administration of IgG4 and GSH augmented the inhibitory effect of IgG4 on the classic ADCC, ADCP, and CDC reactions. Local administration of IgG4/GSH achieved the most obvious effect of accelerating cancer growth in the mouse lung cancer model. The same combination prolonged the survival of skin grafts between two different strains of mouse. In both models, immune cells and several cytokines were found to shift to the state of immune tolerance. CONCLUSION: Combined application of GSH and IgG4 can promote tumor growth and protect skin graft. The mechanism may be achieved through the effect of the Fc-Fc reaction between IgG4 and other tissue-bound IgG subtypes resulting in local immunosuppression. This reaction was facilitated by increased GSH to dissociate the two heavy chains of IgG4 Fc fragment at its disulfide bonds. Our findings unveiled the interaction between the redox system and the immune systems in cancer microenvironment. It offers a sensible explanation for HPD and provides new possibilities for manipulating this mechanism for cancer immunotherapy. Elsevier 2023-01-16 /pmc/articles/PMC9868885/ /pubmed/36681047 http://dx.doi.org/10.1016/j.redox.2023.102608 Text en © 2023 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research Paper
Zhang, Weifeng
Quan, Yan
Ma, Xiaonan
Zeng, Liting
Li, Jirui
Chen, Shuqi
Su, Meng
Hong, Liangli
Li, Penghao
Wang, Hui
Xu, Qian
Zhao, Chanyuan
Zhu, Xiaoqing
Geng, Yiqun
Yan, Xiaomiao
Fang, Zheng
Chen, Muwang
Tian, Dongping
Su, Min
Chen, Xueling
Gu, Jiang
Synergistic effect of glutathione and IgG4 in immune evasion and the implication for cancer immunotherapy()
title Synergistic effect of glutathione and IgG4 in immune evasion and the implication for cancer immunotherapy()
title_full Synergistic effect of glutathione and IgG4 in immune evasion and the implication for cancer immunotherapy()
title_fullStr Synergistic effect of glutathione and IgG4 in immune evasion and the implication for cancer immunotherapy()
title_full_unstemmed Synergistic effect of glutathione and IgG4 in immune evasion and the implication for cancer immunotherapy()
title_short Synergistic effect of glutathione and IgG4 in immune evasion and the implication for cancer immunotherapy()
title_sort synergistic effect of glutathione and igg4 in immune evasion and the implication for cancer immunotherapy()
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9868885/
https://www.ncbi.nlm.nih.gov/pubmed/36681047
http://dx.doi.org/10.1016/j.redox.2023.102608
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