LYVE-1+ macrophages form a collaborative CCR5-dependent perivascular niche that influences chemotherapy responses in murine breast cancer

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Anstee, Joanne, E | Feehan, Karen, T | Opzoomer, James, W | Dean, Isaac | Muller, Henrike, P | Bahri, Meriem | Cheung, Tik Shing | Liakath-Ali, Kifayathullah | Liu, Ziyan | Choy, Desmond | Caron, Jonathan | Sosnowska, Dominika | Beatson, Richard | Muliaditan, Tamara | An, Zhengwen | Gillett, Cheryl, E | Lan, Guocheng | Zou, Xiangang | Watt, Fiona, M | Ng, Tony | Burchell, Joy, M | Kordasti, Shahram | Withers, David, R | Lawrence, Toby | Arnold, James, N

Edité par CCSD ; Elsevier -

International audience. Tumor-associated macrophages (TAMs) are a heterogeneous population of cells that facilitate cancer progression. However, our knowledge of the niches of individual TAM subsets and their development and function remain incomplete. Here, we describe a population of lymphatic vessel endothelial hyaluronan receptor-1 (LYVE-1)-expressing TAMs, which form coordinated multi-cellular “nest” structures that are heterogeneously distributed proximal to vasculature in tumors of a spontaneous murine model of breast cancer. We demonstrate that LYVE-1+ TAMs develop in response to IL-6, which induces their expression of the immune-suppressive enzyme heme oxygenase-1 and promotes a CCR5-dependent signaling axis, which guides their nest formation. Blocking the development of LYVE-1+ TAMs or their nest structures, using gene-targeted mice, results in an increase in CD8+ T cell recruitment to the tumor and enhanced response to chemotherapy. This study highlights an unappreciated collaboration of a TAM subset to form a coordinated niche linked to immune exclusion and resistance to anti-cancer therapy.

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