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Tissue-resident macrophages are major tumor-associated macrophage resources, contributing to early TNBC development, recurrence, and metastases

Ryuichiro Hirano, Koki Okamoto, Miyu Shinke, Marika Sato, S. Watanabe, Hitomi Watanabe, Gen Kondoh, Tetsuya Kadonosono, Shinae Kizaka‐Kondoh

2023Communications Biology54 citationsDOIOpen Access PDF

Abstract

Triple-negative breast cancer (TNBC) is an aggressive and highly heterogenous disease with no well-defined therapeutic targets. Treatment options are thus limited and mortality is significantly higher compared with other breast cancer subtypes. Mammary gland tissue-resident macrophages (MGTRMs) are found to be the most abundant stromal cells in early TNBC before angiogenesis. We therefore aimed to explore novel therapeutic approaches for TNBC by focusing on MGTRMs. Local depletion of MGTRMs in mammary gland fat pads the day before TNBC cell transplantation significantly reduced tumor growth and tumor-associated macrophage (TAM) infiltration in mice. Furthermore, local depletion of MGTRMs at the site of TNBC resection markedly reduced recurrence and distant metastases, and improved chemotherapy outcomes. This study demonstrates that MGTRMs are a major TAM resource and play pivotal roles in the growth and malignant progression of TNBC. The results highlight a possible novel anti-cancer approach targeting tissue-resident macrophages.

Topics & Concepts

Triple-negative breast cancerStromal cellMedicineBreast cancerAngiogenesisCancer researchOncologyMacrophageInfiltration (HVAC)Mammary glandInternal medicineCancerPathologyBiologyThermodynamicsIn vitroBiochemistryPhysicsImmune cells in cancerCancer Cells and MetastasisCancer, Stress, Anesthesia, and Immune Response
Tissue-resident macrophages are major tumor-associated macrophage resources, contributing to early TNBC development, recurrence, and metastases | Litcius