LAG-3+ Regulatory T Cells Suppress Effector Function of T Cells and Allow Their Proliferation Into Regulatory T Cells

Avijit Dutta; Shi Chuen Miaw; Tse Ching Chen; Chia Shiang Chang; Yu Lin Huang; Yung Chang Lin; Chun Yen Lin; Ching Tai Huang

doi:10.1111/imm.70046

LAG-3⁺ Regulatory T Cells Suppress Effector Function of T Cells and Allow Their Proliferation Into Regulatory T Cells

Avijit Dutta, Shi Chuen Miaw, Tse Ching Chen, Chia Shiang Chang, Yu Lin Huang, Yung Chang Lin, Chun Yen Lin, Ching Tai Huang^*

^*Corresponding author for this work

Research output: Contribution to journal › Journal Article › peer-review

Abstract

LAG-3⁺ regulatory T cells suppress the effector but not the proliferative response of naïve cognate antigen-specific CD4⁺ T cells in vivo. The Th1, Th2, and Th17 machineries in the suppressed CD4⁺ T cells are impaired. Genomic study of the suppressed T cells revealed enhanced T cell receptor signalling with up-regulation of immune checkpoints, including PD-1 and PD-L1, and down-regulation of pro-inflammatory pathways. Although oxidative metabolism is reduced, the suppressed T cells retain proliferative capacity and acquire LAG-3 expression with proliferation. They acquire the capacity of LAG-3⁺ regulatory T cells. They inhibit the IFN-γ response of co-cultured naïve CD4⁺ T cells in vitro. Upon adoptive transfer, they rescue mice from lethal autoimmune pulmonitis in a dose-dependent manner. Our results implied a mechanism for the maintenance of long-lasting antigen-specific tolerance.

Original language	English
Journal	Immunology
Early online date	08 10 2025
DOIs	https://doi.org/10.1111/imm.70046
State	E-pub ahead of print - 08 10 2025

Bibliographical note

Keywords

effector function-suppressed proliferation
hemagglutinin-specific CD4 T cells
infectious tolerance
LAG-3 aTreg cell

Access to Document

10.1111/imm.70046

Cite this

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title = "LAG-3+ Regulatory T Cells Suppress Effector Function of T Cells and Allow Their Proliferation Into Regulatory T Cells",

abstract = "LAG-3+ regulatory T cells suppress the effector but not the proliferative response of na{\"i}ve cognate antigen-specific CD4+ T cells in vivo. The Th1, Th2, and Th17 machineries in the suppressed CD4+ T cells are impaired. Genomic study of the suppressed T cells revealed enhanced T cell receptor signalling with up-regulation of immune checkpoints, including PD-1 and PD-L1, and down-regulation of pro-inflammatory pathways. Although oxidative metabolism is reduced, the suppressed T cells retain proliferative capacity and acquire LAG-3 expression with proliferation. They acquire the capacity of LAG-3+ regulatory T cells. They inhibit the IFN-γ response of co-cultured na{\"i}ve CD4+ T cells in vitro. Upon adoptive transfer, they rescue mice from lethal autoimmune pulmonitis in a dose-dependent manner. Our results implied a mechanism for the maintenance of long-lasting antigen-specific tolerance.",

keywords = "effector function-suppressed proliferation, hemagglutinin-specific CD4 T cells, infectious tolerance, LAG-3 aTreg cell",

author = "Avijit Dutta and Miaw, \{Shi Chuen\} and Chen, \{Tse Ching\} and Chang, \{Chia Shiang\} and Huang, \{Yu Lin\} and Lin, \{Yung Chang\} and Lin, \{Chun Yen\} and Huang, \{Ching Tai\}",

note = "{\textcopyright} 2025 The Author(s). Immunology published by John Wiley \& Sons Ltd.",

year = "2025",

month = oct,

day = "8",

doi = "10.1111/imm.70046",

language = "英语",

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T1 - LAG-3+ Regulatory T Cells Suppress Effector Function of T Cells and Allow Their Proliferation Into Regulatory T Cells

AU - Dutta, Avijit

AU - Miaw, Shi Chuen

AU - Chen, Tse Ching

AU - Chang, Chia Shiang

AU - Huang, Yu Lin

AU - Lin, Yung Chang

AU - Lin, Chun Yen

AU - Huang, Ching Tai

PY - 2025/10/8

Y1 - 2025/10/8

N2 - LAG-3+ regulatory T cells suppress the effector but not the proliferative response of naïve cognate antigen-specific CD4+ T cells in vivo. The Th1, Th2, and Th17 machineries in the suppressed CD4+ T cells are impaired. Genomic study of the suppressed T cells revealed enhanced T cell receptor signalling with up-regulation of immune checkpoints, including PD-1 and PD-L1, and down-regulation of pro-inflammatory pathways. Although oxidative metabolism is reduced, the suppressed T cells retain proliferative capacity and acquire LAG-3 expression with proliferation. They acquire the capacity of LAG-3+ regulatory T cells. They inhibit the IFN-γ response of co-cultured naïve CD4+ T cells in vitro. Upon adoptive transfer, they rescue mice from lethal autoimmune pulmonitis in a dose-dependent manner. Our results implied a mechanism for the maintenance of long-lasting antigen-specific tolerance.

AB - LAG-3+ regulatory T cells suppress the effector but not the proliferative response of naïve cognate antigen-specific CD4+ T cells in vivo. The Th1, Th2, and Th17 machineries in the suppressed CD4+ T cells are impaired. Genomic study of the suppressed T cells revealed enhanced T cell receptor signalling with up-regulation of immune checkpoints, including PD-1 and PD-L1, and down-regulation of pro-inflammatory pathways. Although oxidative metabolism is reduced, the suppressed T cells retain proliferative capacity and acquire LAG-3 expression with proliferation. They acquire the capacity of LAG-3+ regulatory T cells. They inhibit the IFN-γ response of co-cultured naïve CD4+ T cells in vitro. Upon adoptive transfer, they rescue mice from lethal autoimmune pulmonitis in a dose-dependent manner. Our results implied a mechanism for the maintenance of long-lasting antigen-specific tolerance.

KW - effector function-suppressed proliferation

KW - hemagglutinin-specific CD4 T cells

KW - infectious tolerance

KW - LAG-3 aTreg cell

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