Author/Authors :
Dung-Fang Lee، نويسنده , , Hsu-Ping Kuo، نويسنده , , Chun-Te Chen، نويسنده , , Jung-Mao Hsu، نويسنده , , Chao-Kai Chou، نويسنده , , Yongkun Wei، نويسنده , , Hui-Lung Sun، نويسنده , , Long-yuan Li، نويسنده , , Bo-Ping Zhang، نويسنده , , Wei-Chien Huang، نويسنده , , Xianghuo He، نويسنده , , Jen-Yu Hung، نويسنده , , Chien-Chen Lai، نويسنده , , Qingqing Ding، نويسنده , , Jen-Liang Su، نويسنده , , Jer-Yen Yang، نويسنده , , Aysegul A. Sahin، نويسنده , , Gabriel N. Hortobagyi، نويسنده , , Fuu-Jen Tsai، نويسنده , , Chang-Hai Tsai، نويسنده , , et al.، نويسنده ,
Abstract :
TNFα has recently emerged as a regulator linking inflammation to cancer pathogenesis, but the detailed cellular and molecular mechanisms underlying this link remain to be elucidated. The tuberous sclerosis 1 (TSC1)/TSC2 tumor suppressor complex serves as a repressor of the mTOR pathway, and disruption of TSC1/TSC2 complex function may contribute to tumorigenesis. Here we show that IKKβ, a major downstream kinase in the TNFα signaling pathway, physically interacts with and phosphorylates TSC1 at Ser487 and Ser511, resulting in suppression of TSC1. The IKKβ-mediated TSC1 suppression activates the mTOR pathway, enhances angiogenesis, and results in tumor development. We further find that expression of activated IKKβ is associated with TSC1 Ser511 phosphorylation and VEGF production in multiple tumor types and correlates with poor clinical outcome of breast cancer patients. Our findings identify a pathway that is critical for inflammation-mediated tumor angiogenesis and may provide a target for clinical intervention in human cancer.