T-regulatory (Treg) cells play a major role in cancer by suppressing protective antitumor immune responses. A series of observations (from a single laboratory) suggest that Treg cells are protective in cancer by virtue of their ability to control cancer-associated inflammation in an interleukin (IL)-10-dependent manner. Here, we report that the ability of Treg cells to produce IL-10 and control inflammation is lost in the course of progressive disease in a mouse model of hereditary colon cancer. Treg cells that expand in adenomatous polyps no longer produce IL-10 and instead switch to production of IL-17. Aberrant Treg cells from polyp-ridden mice promote rather than suppress focal mastocytosis, a critical tumor-promoting inflammatory response. The cells, however, maintain other Treg characteristics, including their inability to produce IL-2 and ability to suppress proliferation of stimulated CD4 T cells. By promoting inflammation and suppressing T-helper functions, these cells act as a double-edged knife propagating tumor growth.
T-regulatory cells shift from a protective anti-inflammatory to a cancer-promoting proinflammatory phenotype in polyposis.
在息肉病中,T调节细胞从具有保护作用的抗炎表型转变为促进癌症发生的促炎表型
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作者:Gounaris Elias, Blatner Nichole R, Dennis Kristen, Magnusson Fay, Gurish Michael F, Strom Terry B, Beckhove Philipp, Gounari Fotini, Khazaie Khashayarsha
| 期刊: | Cancer Research | 影响因子: | 16.600 |
| 时间: | 2009 | 起止号: | 2009 Jul 1; 69(13):5490-7 |
| doi: | 10.1158/0008-5472.CAN-09-0304 | 研究方向: | 细胞生物学 |
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