It is widely accepted that the tumor microenvironment (TUMIC) plays a major role in cancer and is indispensable for tumor progression. The TUMIC involves many "players" going well beyond the malignant-transformed cells, including stromal, immune, and endothelial cells (ECs). The non-malignant cells can acquire tumor-promoting functions during carcinogenesis. In particular, these cells can "orchestrate" the "symphony" of the angiogenic switch, permitting the creation of new blood vessels that allows rapid expansion and progression toward malignancy. Considerable attention within the context of tumor angiogenesis should focus not only on the ECs, representing a fundamental unit, but also on immune cells and on the inflammatory tumor infiltrate. Immune cells infiltrating tumors typically show a tumor-induced polarization associated with attenuation of anti-tumor functions and generation of pro-tumor activities, among these angiogenesis. Here, we propose a scenario suggesting that the angiogenic switch is an immune switch arising from the pro-angiogenic polarization of immune cells. This view links immunity, inflammation, and angiogenesis to tumor progression. Here, we review the data in the literature and seek to identify the "conductors" of this "orchestra." We also suggest that interrupting the immune ? inflammation ? angiogenesis ? tumor progression process can delay or prevent tumor insurgence and malignant disease. © 2014 Bruno, Pagani, Pulze, Albini, Dallaglio, Noonan and Mortara

Bruno, A., Pagani, A., Pulze, L., Albini, A., Dallaglio, K., Noonan M., D., et al. (2014). Orchestration of angiogenesis by immune cells. FRONTIERS IN ONCOLOGY, 4 [10.3389/fonc.2014.00131].

Orchestration of angiogenesis by immune cells

Albini, Adriana;
2014

Abstract

It is widely accepted that the tumor microenvironment (TUMIC) plays a major role in cancer and is indispensable for tumor progression. The TUMIC involves many "players" going well beyond the malignant-transformed cells, including stromal, immune, and endothelial cells (ECs). The non-malignant cells can acquire tumor-promoting functions during carcinogenesis. In particular, these cells can "orchestrate" the "symphony" of the angiogenic switch, permitting the creation of new blood vessels that allows rapid expansion and progression toward malignancy. Considerable attention within the context of tumor angiogenesis should focus not only on the ECs, representing a fundamental unit, but also on immune cells and on the inflammatory tumor infiltrate. Immune cells infiltrating tumors typically show a tumor-induced polarization associated with attenuation of anti-tumor functions and generation of pro-tumor activities, among these angiogenesis. Here, we propose a scenario suggesting that the angiogenic switch is an immune switch arising from the pro-angiogenic polarization of immune cells. This view links immunity, inflammation, and angiogenesis to tumor progression. Here, we review the data in the literature and seek to identify the "conductors" of this "orchestra." We also suggest that interrupting the immune ? inflammation ? angiogenesis ? tumor progression process can delay or prevent tumor insurgence and malignant disease. © 2014 Bruno, Pagani, Pulze, Albini, Dallaglio, Noonan and Mortara
Articolo in rivista - Articolo scientifico
Angiogenesis; Angiogenic switch; Immune cells; Inflammation; Oncology; Cancer Research
English
2014
4
131
none
Bruno, A., Pagani, A., Pulze, L., Albini, A., Dallaglio, K., Noonan M., D., et al. (2014). Orchestration of angiogenesis by immune cells. FRONTIERS IN ONCOLOGY, 4 [10.3389/fonc.2014.00131].
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10281/216817
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