The FoxO4/DKK3 axis represses IFN-γ expression by Th1 cells and limits antimicrobial immunity

Xiang Chen; Jia Hu; Yunfei Wang; Younghee Lee; Xiaohong Zhao; Huiping Lu; Gengzhen Zhu; Hui Wang; Yu Jiang; Fan Liu; Yongzhen Chen; Byung Seok Kim; Qinghua Zhou; Xindong Liu; Xiaohu Wang; Seon Hee Chang; Chen Dong

doi:10.1172/JCI147120

The FoxO4/DKK3 axis represses IFN-γ expression by Th1 cells and limits antimicrobial immunity

Xiang Chen, Jia Hu, Yunfei Wang, Younghee Lee, Xiaohong Zhao, Huiping Lu, Gengzhen Zhu, Hui Wang, Yu Jiang, Fan Liu, Yongzhen Chen, Byung Seok Kim, Qinghua Zhou, Xindong Liu, Xiaohu Wang, Seon Hee Chang, Chen Dong

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4 Scopus citations

Abstract

Forkhead box O transcriptional factors, especially FoxO1 and FoxO3a, play critical roles in physiologic and pathologic immune responses. However, the function of FoxO4, another main member of the FoxO family, in lymphoid cells is still poorly understood. Here, we showed that loss of FoxO4 in T cells augmented IFN-γ production of Th1 cells in vitro. Correspondingly, conditional deletion of FoxO4 in CD4+ T cells enhanced T cell–specific responses to Listeria monocytogenes infection in vivo. Genome-wide occupancy and transcriptomic analyses identified Dkk3 (encoding the Dickkopf-3 protein) as a direct transcriptional target of FoxO4. Consistent with the FoxO4-DKK3 relationship, recombinant DKK3 protein restored normal levels of IFN-γ production in FoxO4-deficient Th1 cells through the downregulation of lymphoid enhancer–binding factor 1 (Lef1) expression. Together, our data suggest a potential FoxO4/DKK3 axis in Th1 cell differentiation, providing what we believe to be an important insight and supplement for FoxO family proteins in T lymphocyte biology and revealing a promising target for the treatment of immune-related diseases.

Original language	English (US)
Article number	e147566
Journal	Journal of Clinical Investigation
Volume	132
Issue number	18
DOIs	https://doi.org/10.1172/JCI147120
State	Published - Sep 15 2022

ASJC Scopus subject areas

General Medicine

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10.1172/JCI147120

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title = "The FoxO4/DKK3 axis represses IFN-γ expression by Th1 cells and limits antimicrobial immunity",

abstract = "Forkhead box O transcriptional factors, especially FoxO1 and FoxO3a, play critical roles in physiologic and pathologic immune responses. However, the function of FoxO4, another main member of the FoxO family, in lymphoid cells is still poorly understood. Here, we showed that loss of FoxO4 in T cells augmented IFN-γ production of Th1 cells in vitro. Correspondingly, conditional deletion of FoxO4 in CD4+ T cells enhanced T cell–specific responses to Listeria monocytogenes infection in vivo. Genome-wide occupancy and transcriptomic analyses identified Dkk3 (encoding the Dickkopf-3 protein) as a direct transcriptional target of FoxO4. Consistent with the FoxO4-DKK3 relationship, recombinant DKK3 protein restored normal levels of IFN-γ production in FoxO4-deficient Th1 cells through the downregulation of lymphoid enhancer–binding factor 1 (Lef1) expression. Together, our data suggest a potential FoxO4/DKK3 axis in Th1 cell differentiation, providing what we believe to be an important insight and supplement for FoxO family proteins in T lymphocyte biology and revealing a promising target for the treatment of immune-related diseases.",

author = "Xiang Chen and Jia Hu and Yunfei Wang and Younghee Lee and Xiaohong Zhao and Huiping Lu and Gengzhen Zhu and Hui Wang and Yu Jiang and Fan Liu and Yongzhen Chen and Kim, {Byung Seok} and Qinghua Zhou and Xindong Liu and Xiaohu Wang and Chang, {Seon Hee} and Chen Dong",

note = "Publisher Copyright: {\textcopyright} 2022, Chen et al. This is an open access article published under the terms of the Creative Commons Attribution 4.0 International License.",

year = "2022",

month = sep,

day = "15",

doi = "10.1172/JCI147120",

language = "English (US)",

volume = "132",

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T1 - The FoxO4/DKK3 axis represses IFN-γ expression by Th1 cells and limits antimicrobial immunity

AU - Chen, Xiang

AU - Hu, Jia

AU - Wang, Yunfei

AU - Lee, Younghee

AU - Zhao, Xiaohong

AU - Lu, Huiping

AU - Zhu, Gengzhen

AU - Wang, Hui

AU - Jiang, Yu

AU - Liu, Fan

AU - Chen, Yongzhen

AU - Kim, Byung Seok

AU - Zhou, Qinghua

AU - Liu, Xindong

AU - Wang, Xiaohu

AU - Chang, Seon Hee

AU - Dong, Chen

PY - 2022/9/15

Y1 - 2022/9/15

N2 - Forkhead box O transcriptional factors, especially FoxO1 and FoxO3a, play critical roles in physiologic and pathologic immune responses. However, the function of FoxO4, another main member of the FoxO family, in lymphoid cells is still poorly understood. Here, we showed that loss of FoxO4 in T cells augmented IFN-γ production of Th1 cells in vitro. Correspondingly, conditional deletion of FoxO4 in CD4+ T cells enhanced T cell–specific responses to Listeria monocytogenes infection in vivo. Genome-wide occupancy and transcriptomic analyses identified Dkk3 (encoding the Dickkopf-3 protein) as a direct transcriptional target of FoxO4. Consistent with the FoxO4-DKK3 relationship, recombinant DKK3 protein restored normal levels of IFN-γ production in FoxO4-deficient Th1 cells through the downregulation of lymphoid enhancer–binding factor 1 (Lef1) expression. Together, our data suggest a potential FoxO4/DKK3 axis in Th1 cell differentiation, providing what we believe to be an important insight and supplement for FoxO family proteins in T lymphocyte biology and revealing a promising target for the treatment of immune-related diseases.

AB - Forkhead box O transcriptional factors, especially FoxO1 and FoxO3a, play critical roles in physiologic and pathologic immune responses. However, the function of FoxO4, another main member of the FoxO family, in lymphoid cells is still poorly understood. Here, we showed that loss of FoxO4 in T cells augmented IFN-γ production of Th1 cells in vitro. Correspondingly, conditional deletion of FoxO4 in CD4+ T cells enhanced T cell–specific responses to Listeria monocytogenes infection in vivo. Genome-wide occupancy and transcriptomic analyses identified Dkk3 (encoding the Dickkopf-3 protein) as a direct transcriptional target of FoxO4. Consistent with the FoxO4-DKK3 relationship, recombinant DKK3 protein restored normal levels of IFN-γ production in FoxO4-deficient Th1 cells through the downregulation of lymphoid enhancer–binding factor 1 (Lef1) expression. Together, our data suggest a potential FoxO4/DKK3 axis in Th1 cell differentiation, providing what we believe to be an important insight and supplement for FoxO family proteins in T lymphocyte biology and revealing a promising target for the treatment of immune-related diseases.

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The FoxO4/DKK3 axis represses IFN-γ expression by Th1 cells and limits antimicrobial immunity

Abstract

ASJC Scopus subject areas

MD Anderson CCSG core facilities

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