T cell-but not tumor cell-produced TGF-β1 promotes the development of spontaneous mammary cancer

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Abstract

During their development, tumors acquire multiple capabilities that enable them to proliferate, disseminate and evade immunosurveillance. A putative mechanism is through the production of the cytokine TGF-β1. We showed in our recent studies that T cell-produced TGF-β1 inhibits antitumor T cell responses to foster tumor growth raising the question of the precise function of TGF-β1 produced by tumor cells in tumor development. Here, using a transgenic model of mammary cancer, we report that deletion of TGF-β1 from tumor cells did not protect mice from tumor development. However, ablation of TGF-β1 from T cells significantly inhibited mammary tumor growth. Additionally, absence of TGF-β1 in T cells prevented tumors from advancing to higher pathological grades and further suppressed secondary tumor development in the lungs. These findings reveal T cells but not tumor cells as a critical source of TGF-β1 that promotes tumor development. © Sarkar et al.

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Sarkar, A., Donkor, M. K., & Li, M. O. (2011). T cell-but not tumor cell-produced TGF-β1 promotes the development of spontaneous mammary cancer. Oncotarget, 2(12), 1339–1351. https://doi.org/10.18632/oncotarget.403

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