Macrophages orchestrate breast cancer early dissemination and metastasis

巨噬细胞在乳腺癌早期扩散和转移中发挥主导作用

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作者:Nina Linde ,Maria Casanova-Acebes ,Maria Soledad Sosa ,Arthur Mortha ,Adeeb Rahman ,Eduardo Farias ,Kathryn Harper ,Ethan Tardio ,Ivan Reyes Torres ,Joan Jones ,John Condeelis ,Miriam Merad ,Julio A Aguirre-Ghiso

Abstract

Cancer cell dissemination during very early stages of breast cancer proceeds through poorly understood mechanisms. Here we show, in a mouse model of HER2+ breast cancer, that a previously described sub-population of early-evolved cancer cells requires macrophages for early dissemination. Depletion of macrophages specifically during pre-malignant stages reduces early dissemination and also results in reduced metastatic burden at end stages of cancer progression. Mechanistically, we show that, in pre-malignant lesions, CCL2 produced by cancer cells and myeloid cells attracts CD206+/Tie2+ macrophages and induces Wnt-1 upregulation that in turn downregulates E-cadherin junctions in the HER2+ early cancer cells. We also observe macrophage-containing tumor microenvironments of metastasis structures in the pre-malignant lesions that can operate as portals for intravasation. These data support a causal role for macrophages in early dissemination that affects long-term metastasis development much later in cancer progression. A pilot analysis on human specimens revealed intra-epithelial macrophages and loss of E-cadherin junctions in ductal carcinoma in situ, supporting a potential clinical relevance.

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