Research output: Contribution to journal › Article › peer-review
Anders Etzerodt, Morgane Moulin, Thomas Koed Doktor, Marcello Delfini, Noushine Mossadegh-Keller, Marc Bajenoff, Michael H. Sieweke, Søren Kragh Moestrup, Nathalie Auphan-Anezin, Toby Lawrence
Original language | English |
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Article number | e20191869 |
Journal | The Journal of experimental medicine |
Volume | 217 |
Issue number | 4 |
Early online date | 6 Apr 2020 |
DOIs | |
Accepted/In press | 16 Dec 2019 |
E-pub ahead of print | 6 Apr 2020 |
Published | 6 Apr 2020 |
Additional links |
Tissue_resident_macrophages_in_omentum_promote_LAWRENCE_Publishedonline6April2020_GOLD_VoR_CC_BY_SA_.pdf, 7.86 MB, application/pdf
Uploaded date:22 Mar 2021
Version:Final published version
Licence:CC BY-SA
Experimental and clinical evidence suggests that tumor-associated macrophages (TAMs) play important roles in cancer progression. Here, we have characterized the ontogeny and function of TAM subsets in a mouse model of metastatic ovarian cancer that is representative for visceral peritoneal metastasis. We show that the omentum is a critical premetastatic niche for development of invasive disease in this model and define a unique subset of CD163+ Tim4+ resident omental macrophages responsible for metastatic spread of ovarian cancer cells. Transcriptomic analysis showed that resident CD163+ Tim4+ omental macrophages were phenotypically distinct and maintained their resident identity during tumor growth. Selective depletion of CD163+ Tim4+ macrophages in omentum using genetic and pharmacological tools prevented tumor progression and metastatic spread of disease. These studies describe a specific role for tissue-resident macrophages in the invasive progression of metastatic ovarian cancer. The molecular pathways of cross-talk between tissue-resident macrophages and disseminated cancer cells may represent new targets to prevent metastasis and disease recurrence.
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