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Tumor-induced myeloid deviation: when myeloid-derived suppressor cells meet tumor-associated macrophages
Stefano Ugel, … , Susanna Mandruzzato, Vincenzo Bronte
Stefano Ugel, … , Susanna Mandruzzato, Vincenzo Bronte
Published September 1, 2015
Citation Information: J Clin Invest. 2015;125(9):3365-3376. https://doi.org/10.1172/JCI80006.
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Review Series

Tumor-induced myeloid deviation: when myeloid-derived suppressor cells meet tumor-associated macrophages

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Abstract

The generation of an inflammatory environment is favorable and often decisive for the growth of both primary tumors and metastases. Tumor cells either express membrane molecules or release tumor-derived soluble factors able to alter myelopoiesis. Tumor-reprogrammed myeloid cells not only create a tolerogenic environment by blocking T cell functions and proliferation, but also directly drive tumor growth by promoting cancer stemness, angiogenesis, stroma deposition, epithelial-to-mesenchymal transition, and metastasis formation. In this Review, we discuss the interplay between immunosuppressive and protumoral myeloid cells and detail their immune-regulatory mechanisms, the molecular pathways involved in their differentiation, as well as their potential role as prognostic and diagnostic biomarkers and prospective targets for innovative approaches to treat tumor-bearing hosts.

Authors

Stefano Ugel, Francesco De Sanctis, Susanna Mandruzzato, Vincenzo Bronte

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Synopsis of therapeutic interventions to limit monocyte and macrophage p...

Synopsis of therapeutic interventions to limit monocyte and macrophage protumoral activity


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