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Publication : The cellular and molecular origin of tumor-associated macrophages.

First Author  Franklin RA Year  2014
Journal  Science Volume  344
Issue  6186 Pages  921-5
PubMed ID  24812208 Mgi Jnum  J:212544
Mgi Id  MGI:5581753 Doi  10.1126/science.1252510
Citation  Franklin RA, et al. (2014) The cellular and molecular origin of tumor-associated macrophages. Science 344(6186):921-5
abstractText  Long recognized as an evolutionarily ancient cell type involved in tissue homeostasis and immune defense against pathogens, macrophages are being rediscovered as regulators of several diseases, including cancer. Here we show that in mice, mammary tumor growth induces the accumulation of tumor-associated macrophages (TAMs) that are phenotypically and functionally distinct from mammary tissue macrophages (MTMs). TAMs express the adhesion molecule Vcam1 and proliferate upon their differentiation from inflammatory monocytes, but do not exhibit an "alternatively activated" phenotype. TAM terminal differentiation depends on the transcriptional regulator of Notch signaling, RBPJ; and TAM, but not MTM, depletion restores tumor-infiltrating cytotoxic T cell responses and suppresses tumor growth. These findings reveal the ontogeny of TAMs and a discrete tumor-elicited inflammatory response, which may provide new opportunities for cancer immunotherapy.
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