Cancer stem cell-derived CHI3L1 activates the MAF/CTLA4 signaling pathway to promote immune escape in triple-negative breast cancer

Shufeng Ji; Hao Yu; Dan Zhou; Xulong Fan; Yan Duan; Yijiang Tan; Min Lang; Guoli Shao

doi:10.1186/s12967-023-04532-6

Journal of Translational Medicine (Oct 2023)

Cancer stem cell-derived CHI3L1 activates the MAF/CTLA4 signaling pathway to promote immune escape in triple-negative breast cancer

Shufeng Ji,
Hao Yu,
Dan Zhou,
Xulong Fan,
Yan Duan,
Yijiang Tan,
Min Lang,
Guoli Shao

Affiliations

Shufeng Ji: Special Medical Service Center, General Surgery, Zhujiang Hospital of Southern Medical University
Hao Yu: Special Medical Service Center, General Surgery, Zhujiang Hospital of Southern Medical University
Dan Zhou: Department of Breast Surgery, The First People’s Hospital of Foshan
Xulong Fan: Department of Breast Surgery, Maternity and Children’s Healthcare Hospital of Foshan
Yan Duan: Special Medical Service Center, General Surgery, Zhujiang Hospital of Southern Medical University
Yijiang Tan: Special Medical Service Center, General Surgery, Zhujiang Hospital of Southern Medical University
Min Lang: Special Medical Service Center, General Surgery, Zhujiang Hospital of Southern Medical University
Guoli Shao: Special Medical Service Center, General Surgery, Zhujiang Hospital of Southern Medical University

DOI: https://doi.org/10.1186/s12967-023-04532-6
Journal volume & issue: Vol. 21, no. 1
pp. 1 – 18

Abstract

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Abstract Background Triple-negative breast cancer (TNBC) development may be associated with tumor immune escape. This study explores whether the CHI3L1/MAF/CTLA4/S100A4 axis affects immune escape in TNBC through interplay with triple-negative breast cancer stem cells (TN-BCSCs). Objective The aim of this study is to utilize single-cell transcriptome sequencing (scRNA-seq) to uncover the molecular mechanisms by which the CHI3L1/MAF/CTLA4 signaling pathway may mediate immune evasion in triple-negative breast cancer through the interaction between tumor stem cells (CSCs) and immune cells. Methods Cell subsets in TNBC tissues were obtained through scRNA-seq, followed by screening differentially expressed genes in TN-BCSCs and B.C.s (CD44+ and CD24−) and predicting the transcription factor regulated by CHI3L1. Effect of CHI3L1 on the stemness phenotype of TNBC cells investigated. Effects of BCSCs-231-derived CHI3L1 on CTLA4 expression in T cells were explored after co-culture of BCSCs-231 cells obtained from microsphere culture of TN-BCSCs with T cells. BCSCs-231-treated T cells were co-cultured with CD8+ T cells to explore the resultant effect on T cell cytotoxicity. An orthotopic B.C. transplanted tumor model in mice with humanized immune systems was constructed, in which the Role of CHI3L1/MAF/CTLA4 in the immune escape of TNBC was explored. Results Eight cell subsets were found in the TNBC tissues, and the existence of TN-BCSCs was observed in the epithelial cell subset. CHI3L1 was related to the stemness phenotype of TNBC cells. TN-BCSC-derived CHI3L1 increased CTLA4 expression in T cells through MAF, inhibiting CD8+ T cell cytotoxicity and inducing immunosuppression. Furthermore, the CTLA4+ T cells might secrete S100A4 to promote the stemness phenotype of TNBC cells. Conclusions TN-BCSC-derived CHI3L1 upregulates CTLA4 expression in T cells through MAF, suppressing the function of CD8+ T cells, which promotes the immune escape of TNBC.

Published in Journal of Translational Medicine

ISSN: 1479-5876 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine
Website: https://translational-medicine.biomedcentral.com/

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