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Cell: Lung-resident alveolar macrophages regulate the timing of breast cancer metastasis

作者:   发布于:2026年01月11日  点击量:9
Title:

Lung-resident alveolar macrophages regulate the timing of breast cancer metastasis

Journal:

Cell

Year:

2024

Abstract

Breast disseminated cancer cells (DCCs) can remain dormant in the lungs for extended periods, but the mechanisms limiting their expansion are not well understood. Research indicates that tissue-resident alveolar macrophages suppress breast cancer metastasis in lung alveoli by inducing dormancy. Through ligand-receptor mapping and intravital imaging, it was found that alveolar macrophages express transforming growth factor (TGF)-β2. This expression, along with persistent macrophage-cancer cell interactions via the TGF-βRIII receptor, maintains cancer cells in a dormant state. Depleting alveolar macrophages or losing the TGF-β2 receptor in cancer cells triggers metastatic awakening. Aggressive breast cancer cells are either suppressed by alveolar macrophages or evade this suppression by avoiding interaction and downregulating the TGF-β2 receptor. Restoring TGF-βRIII in aggressive cells reinstates TGF-β2-mediated macrophage growth suppression. Thus, alveolar macrophages act as a metastasis immune barrier, and downregulation of TGF-β2 signaling allows cancer cells to overcome macrophage-mediated growth suppression.

Highlights

•Embryo-derived alveolar macrophages (AMs) induce disseminated cancer cell dormancy

•Disseminated cancer cells (DCCs) interact frequently with AMs in the lung alveolus

•DCC dormancy is due to persistent AM-DCC interactions via TGF-β2-TGF-βRIII signaling

•Loss of AMs or TGF-βRIII in DCCs eliminates an innate immune barrier to metastasis

Cite

20240812-cell-Liposoma-Data

20240812-cell-Liposoma-MM







Links
https://www.cell.com/cell/fulltext/S0092-8674(24)01034-1(如需全文,请联系我们)