Post-translational Modification of PD-1: Potential Targets for Cancer Immunotherapy

Te An Lee; En Yun Tsai; Shou Hou Liu; Shih Duo Hsu Hung; Shing Jyh Chang; Chi Hong Chao; Yun Ju Lai; Hirohito Yamaguchi; Chia Wei Li

doi:10.1158/0008-5472.CAN-23-2664

Post-translational Modification of PD-1: Potential Targets for Cancer Immunotherapy

Te An Lee, En Yun Tsai, Shou Hou Liu, Shih Duo Hsu Hung, Shing Jyh Chang, Chi Hong Chao, Yun Ju Lai, Hirohito Yamaguchi, Chia Wei Li^*

^*此作品的通信作者

研究成果: Review article › 同行評審

17 引文斯高帕斯（Scopus）

摘要

Activation of effector T cells leads to upregulation of PD-1, which can inhibit T-cell activity following engagement with its ligand PD-L1. Post-translational modifications (PTM), including glycosylation, phosphorylation, ubiquitination, and palmitoylation, play a significant role in regulating PD-1 protein stability, localization, and interprotein interactions. Targeting PTM of PD-1 in T cells has emerged as a potential strategy to overcome PD-1–mediated immunosuppression in cancer and enhances antitumor immunity. The regulatory signaling pathways that induce PTM of PD-1 can be suppressed with small-molecule inhibitors, and mAbs can directly target PD-1 PTMs. Preliminary outcomes from exploratory studies suggest that focusing on the PTM of PD-1 has strong therapeutic potential and can enhance the response to anti-PD-1.

原文	English
頁（從 - 到）	800-807
頁數	8
期刊	Cancer Research
卷	84
發行號	6
DOIs	https://doi.org/10.1158/0008-5472.CAN-23-2664
出版狀態	Published - 15 3月 2024

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title = "Post-translational Modification of PD-1: Potential Targets for Cancer Immunotherapy",

abstract = "Activation of effector T cells leads to upregulation of PD-1, which can inhibit T-cell activity following engagement with its ligand PD-L1. Post-translational modifications (PTM), including glycosylation, phosphorylation, ubiquitination, and palmitoylation, play a significant role in regulating PD-1 protein stability, localization, and interprotein interactions. Targeting PTM of PD-1 in T cells has emerged as a potential strategy to overcome PD-1–mediated immunosuppression in cancer and enhances antitumor immunity. The regulatory signaling pathways that induce PTM of PD-1 can be suppressed with small-molecule inhibitors, and mAbs can directly target PD-1 PTMs. Preliminary outcomes from exploratory studies suggest that focusing on the PTM of PD-1 has strong therapeutic potential and can enhance the response to anti-PD-1.",

author = "Lee, {Te An} and Tsai, {En Yun} and Liu, {Shou Hou} and Hung, {Shih Duo Hsu} and Chang, {Shing Jyh} and Chao, {Chi Hong} and Lai, {Yun Ju} and Hirohito Yamaguchi and Li, {Chia Wei}",

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T2 - Potential Targets for Cancer Immunotherapy

AU - Lee, Te An

AU - Tsai, En Yun

AU - Liu, Shou Hou

AU - Hung, Shih Duo Hsu

AU - Chang, Shing Jyh

AU - Chao, Chi Hong

AU - Lai, Yun Ju

AU - Yamaguchi, Hirohito

AU - Li, Chia Wei

PY - 2024/3/15

Y1 - 2024/3/15

N2 - Activation of effector T cells leads to upregulation of PD-1, which can inhibit T-cell activity following engagement with its ligand PD-L1. Post-translational modifications (PTM), including glycosylation, phosphorylation, ubiquitination, and palmitoylation, play a significant role in regulating PD-1 protein stability, localization, and interprotein interactions. Targeting PTM of PD-1 in T cells has emerged as a potential strategy to overcome PD-1–mediated immunosuppression in cancer and enhances antitumor immunity. The regulatory signaling pathways that induce PTM of PD-1 can be suppressed with small-molecule inhibitors, and mAbs can directly target PD-1 PTMs. Preliminary outcomes from exploratory studies suggest that focusing on the PTM of PD-1 has strong therapeutic potential and can enhance the response to anti-PD-1.

AB - Activation of effector T cells leads to upregulation of PD-1, which can inhibit T-cell activity following engagement with its ligand PD-L1. Post-translational modifications (PTM), including glycosylation, phosphorylation, ubiquitination, and palmitoylation, play a significant role in regulating PD-1 protein stability, localization, and interprotein interactions. Targeting PTM of PD-1 in T cells has emerged as a potential strategy to overcome PD-1–mediated immunosuppression in cancer and enhances antitumor immunity. The regulatory signaling pathways that induce PTM of PD-1 can be suppressed with small-molecule inhibitors, and mAbs can directly target PD-1 PTMs. Preliminary outcomes from exploratory studies suggest that focusing on the PTM of PD-1 has strong therapeutic potential and can enhance the response to anti-PD-1.

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SN - 0008-5472

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SP - 800

EP - 807

JO - Cancer Research

JF - Cancer Research

IS - 6

ER -

Post-translational Modification of PD-1: Potential Targets for Cancer Immunotherapy

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