Tumor-migrating peripheral Foxp3-high regulatory T cells drive poor prognosis in hepatocellular carcinoma

CD4+ regulatory T cells (Tregs) are pivotal in HCC progression. However, systemic depletion of all Tregs risks autoimmunity. Existing subgroup classifications highlight Tregs' phenotypic and functional heterogeneity but lack coherent consensus. This study aimed to classify Treg subtypes using s...

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Published in:Hepatology (Baltimore, Md.)
Main Authors: Huang, Chien-Hao, Ku, Wei-Ting, Mahalingam, Jayashri, Wu, Cheng-Heng, Wu, Tsung-Han, Fan, Jian-He, Su, Chung-Wei, Lin, Po-Ting, Peng, Chien-Wei, Yang, Chan-Keng, Teng, Wei, Jeng, Wen-Juei, Chen, Wei-Ting, Lin, Chen-Chun, Lin, Shi-Ming, Sheen, I-Shyan, Lin, Yung-Chang, Lin, Chun-Yen
Format: Journal Article
Language:English
Published: 01.07.2025
ISSN:1527-3350, 1527-3350
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Abstract CD4+ regulatory T cells (Tregs) are pivotal in HCC progression. However, systemic depletion of all Tregs risks autoimmunity. Existing subgroup classifications highlight Tregs' phenotypic and functional heterogeneity but lack coherent consensus. This study aimed to classify Treg subtypes using single-cell CITE-seq, integrating data from tumor, non-tumor, and blood samples in HCC patients. We also validated the clinical relevance and prognostic value of this classification.BACKGROUND AND AIMSCD4+ regulatory T cells (Tregs) are pivotal in HCC progression. However, systemic depletion of all Tregs risks autoimmunity. Existing subgroup classifications highlight Tregs' phenotypic and functional heterogeneity but lack coherent consensus. This study aimed to classify Treg subtypes using single-cell CITE-seq, integrating data from tumor, non-tumor, and blood samples in HCC patients. We also validated the clinical relevance and prognostic value of this classification.CITE-seq analysis was performed on 51,067 CD4+ T cells from eight HCC patients. Validation involved 96 HCC patients and 53 healthy donors using flow cytometry, functional assays, and clinical data.METHODSCITE-seq analysis was performed on 51,067 CD4+ T cells from eight HCC patients. Validation involved 96 HCC patients and 53 healthy donors using flow cytometry, functional assays, and clinical data.Trajectory and TCR analyses identified a peripheral Foxp3high Treg subset that preferentially migrate to tumor sites, acquiring a terminally differentiated, activated phenotype. These tumor-infiltrating Foxp3high Tregs exhibit elevated LAYN and TRM signatures and further increase their Foxp3 expression and immunosuppressive functions by pro-inflammatory cytokines in tumor tissue. The CCL5/CCR5 axis is crucial for recruiting Foxp3high Tregs from peripheral blood into the tumor microenvironment. A strong correlation was observed between the percentage of Foxp3high Tregs in peripheral blood and their counterparts in tumor regions, suggesting their potential as peripheral biomarker. Notably, a peripheral Foxp3high Tregs/CD4+ T cells percentage>3.5% predicted overall survival and early recurrence, with AUROCs exceeding 0.75.RESULTSTrajectory and TCR analyses identified a peripheral Foxp3high Treg subset that preferentially migrate to tumor sites, acquiring a terminally differentiated, activated phenotype. These tumor-infiltrating Foxp3high Tregs exhibit elevated LAYN and TRM signatures and further increase their Foxp3 expression and immunosuppressive functions by pro-inflammatory cytokines in tumor tissue. The CCL5/CCR5 axis is crucial for recruiting Foxp3high Tregs from peripheral blood into the tumor microenvironment. A strong correlation was observed between the percentage of Foxp3high Tregs in peripheral blood and their counterparts in tumor regions, suggesting their potential as peripheral biomarker. Notably, a peripheral Foxp3high Tregs/CD4+ T cells percentage>3.5% predicted overall survival and early recurrence, with AUROCs exceeding 0.75.Peripheral Foxp3high Tregs migrate to tumor sites via the CCR5-CCL5 axis and mature in response to pro-inflammatory cytokines. The proportion of these Tregs in peripheral blood correlates with their presence in tumors, making them a potential biomarker for predicting HCC outcomes.CONCLUSIONPeripheral Foxp3high Tregs migrate to tumor sites via the CCR5-CCL5 axis and mature in response to pro-inflammatory cytokines. The proportion of these Tregs in peripheral blood correlates with their presence in tumors, making them a potential biomarker for predicting HCC outcomes.
AbstractList CD4+ regulatory T cells (Tregs) are pivotal in HCC progression. However, systemic depletion of all Tregs risks autoimmunity. Existing subgroup classifications highlight Tregs' phenotypic and functional heterogeneity but lack coherent consensus. This study aimed to classify Treg subtypes using single-cell CITE-seq, integrating data from tumor, non-tumor, and blood samples in HCC patients. We also validated the clinical relevance and prognostic value of this classification.BACKGROUND AND AIMSCD4+ regulatory T cells (Tregs) are pivotal in HCC progression. However, systemic depletion of all Tregs risks autoimmunity. Existing subgroup classifications highlight Tregs' phenotypic and functional heterogeneity but lack coherent consensus. This study aimed to classify Treg subtypes using single-cell CITE-seq, integrating data from tumor, non-tumor, and blood samples in HCC patients. We also validated the clinical relevance and prognostic value of this classification.CITE-seq analysis was performed on 51,067 CD4+ T cells from eight HCC patients. Validation involved 96 HCC patients and 53 healthy donors using flow cytometry, functional assays, and clinical data.METHODSCITE-seq analysis was performed on 51,067 CD4+ T cells from eight HCC patients. Validation involved 96 HCC patients and 53 healthy donors using flow cytometry, functional assays, and clinical data.Trajectory and TCR analyses identified a peripheral Foxp3high Treg subset that preferentially migrate to tumor sites, acquiring a terminally differentiated, activated phenotype. These tumor-infiltrating Foxp3high Tregs exhibit elevated LAYN and TRM signatures and further increase their Foxp3 expression and immunosuppressive functions by pro-inflammatory cytokines in tumor tissue. The CCL5/CCR5 axis is crucial for recruiting Foxp3high Tregs from peripheral blood into the tumor microenvironment. A strong correlation was observed between the percentage of Foxp3high Tregs in peripheral blood and their counterparts in tumor regions, suggesting their potential as peripheral biomarker. Notably, a peripheral Foxp3high Tregs/CD4+ T cells percentage>3.5% predicted overall survival and early recurrence, with AUROCs exceeding 0.75.RESULTSTrajectory and TCR analyses identified a peripheral Foxp3high Treg subset that preferentially migrate to tumor sites, acquiring a terminally differentiated, activated phenotype. These tumor-infiltrating Foxp3high Tregs exhibit elevated LAYN and TRM signatures and further increase their Foxp3 expression and immunosuppressive functions by pro-inflammatory cytokines in tumor tissue. The CCL5/CCR5 axis is crucial for recruiting Foxp3high Tregs from peripheral blood into the tumor microenvironment. A strong correlation was observed between the percentage of Foxp3high Tregs in peripheral blood and their counterparts in tumor regions, suggesting their potential as peripheral biomarker. Notably, a peripheral Foxp3high Tregs/CD4+ T cells percentage>3.5% predicted overall survival and early recurrence, with AUROCs exceeding 0.75.Peripheral Foxp3high Tregs migrate to tumor sites via the CCR5-CCL5 axis and mature in response to pro-inflammatory cytokines. The proportion of these Tregs in peripheral blood correlates with their presence in tumors, making them a potential biomarker for predicting HCC outcomes.CONCLUSIONPeripheral Foxp3high Tregs migrate to tumor sites via the CCR5-CCL5 axis and mature in response to pro-inflammatory cytokines. The proportion of these Tregs in peripheral blood correlates with their presence in tumors, making them a potential biomarker for predicting HCC outcomes.
Author Lin, Yung-Chang
Fan, Jian-He
Jeng, Wen-Juei
Teng, Wei
Lin, Chun-Yen
Mahalingam, Jayashri
Wu, Cheng-Heng
Ku, Wei-Ting
Lin, Po-Ting
Lin, Chen-Chun
Lin, Shi-Ming
Wu, Tsung-Han
Su, Chung-Wei
Peng, Chien-Wei
Chen, Wei-Ting
Huang, Chien-Hao
Yang, Chan-Keng
Sheen, I-Shyan
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