Immunotherapeutic IL-6R and targeting the MCT-1/IL-6/CXCL7/PD-L1 circuit prevent relapse and metastasis of triple-negative breast cancer

Aushia Tanzih Al Haq; Pao-Pao Yang; Christopher Jin; Jou-Ho Shih; Li-Mei Chen; Hong-Yu Tseng; Yen-An Chen; Yueh-Shan Weng; Lu-Hai Wang; Michael P Snyder; Hsin-Ling Hsu

doi:10.7150/thno.92922

Immunotherapeutic IL-6R and targeting the MCT-1/IL-6/CXCL7/PD-L1 circuit prevent relapse and metastasis of triple-negative breast cancer

Theranostics. 2024 Mar 3;14(5):2167-2189. doi: 10.7150/thno.92922. eCollection 2024.

Authors

Affiliations

¹ Institute of Molecular and Genomic Medicine, National Health Research Institutes, Miaoli, Taiwan.
² Department of Genetics, Stanford University School of Medicine, Stanford, CA, USA.
³ Institute of Integrated Medicine and Chinese Medicine Research Center, China Medical University, Taichung, Taiwan.

Abstract

Rationale: Multiple copies in T-cell malignancy 1 (MCT-1) is a prognostic biomarker for aggressive breast cancers. Overexpressed MCT-1 stimulates the IL-6/IL-6R/gp130/STAT3 axis, which promotes epithelial-to-mesenchymal transition and cancer stemness. Because cancer stemness largely contributes to the tumor metastasis and recurrence, we aimed to identify whether the blockade of MCT-1 and IL-6R can render these effects and to understand the underlying mechanisms that govern the process. Methods: We assessed primary tumor invasion, postsurgical local recurrence and distant metastasis in orthotopic syngeneic mice given the indicated immunotherapy and MCT-1 silencing (shMCT-1). Results: We found that shMCT-1 suppresses the transcriptomes of the inflammatory response and metastatic signaling in TNBC cells and inhibits tumor recurrence, metastasis and mortality in xenograft mice. IL-6R immunotherapy and shMCT-1 combined further decreased intratumoral M2 macrophages and T regulatory cells (Tregs) and avoided postsurgical TNBC expansion. shMCT-1 also enhances IL-6R-based immunotherapy effectively in preventing postsurgical TNBC metastasis, recurrence and mortality. Anti-IL-6R improved helper T, cytotoxic T and natural killer (NK) cells in the lymphatic system and decreased Tregs in the recurrent and metastatic tumors. Combined IL-6R and PD-L1 immunotherapies abridged TNBC cell stemness and M2 macrophage activity to a greater extent than monotherapy. Sequential immunotherapy of PD-L1 and IL-6R demonstrated the best survival outcome and lowest postoperative recurrence and metastasis compared with synchronized therapy, particularly in the shMCT-1 context. Multiple positive feedforward loops of the MCT-1/IL-6/IL-6R/CXCL7/PD-L1 axis were identified in TNBC cells, which boosted metastatic niches and immunosuppressive microenvironments. Clinically, MCT-1^high/PD-L1^high/CXCL7^high and CXCL7^high/IL-6^high/IL-6R^high expression patterns predict worse prognosis and poorer survival of breast cancer patients. Conclusion: Systemic targeting the MCT-1/IL-6/IL-6R/CXCL7/PD-L1 interconnections enhances immune surveillance that inhibits the aggressiveness of TNBC.

Keywords: CXCL7/CXCR2; IL-6/IL-6R; Immunotherapy; MCT-1; PD-L1.

MeSH terms

Animals
B7-H1 Antigen* / metabolism
Cell Line, Tumor
Humans
Immunotherapy
Interleukin-6 / metabolism
Mice
Neoplasm Recurrence, Local / prevention & control
Triple Negative Breast Neoplasms* / drug therapy
Tumor Microenvironment

Substances

B7-H1 Antigen
Interleukin-6

Grants and funding

U2C CA233311/CA/NCI NIH HHS/United States