Here, we provide evidence for a functional role of artemin (ARTN) in progression of endometrial carcinoma (EC). Increased ARTN protein expression was observed in EC compared with normal endometrial tissue, and ARTN protein expression in EC was significantly associated with higher tumor grade and invasiveness. Forced expression of ARTN in EC cells significantly increased total cell number as a result of enhanced cell cycle progression and cell survival. In addition, forced expression of ARTN significantly enhanced anchorage-independent growth and invasiveness of EC cells. Moreover, forced expression of ARTN increased tumor size in xenograft models and produced highly proliferative, poorly differentiated, and invasive tumors. The ARTN-stimulated increases in oncogenicity and invasion were mediated by increased expression and activity of AKT1. Small interfering RNA-mediated depletion or antibody inhibition of ARTN significantly reduced oncogenicity and invasion of EC cells. Thus, inhibition of ARTN may be considered as a potential therapeutic strategy to retard progression of EC.
Vijay Pandey, Yewon Jung, Jian Jian Kang, Michael Steiner, Pengxu Qian, Arindam Banerjee, Murray D. Mitchell, Zhengsheng Wu, Tao Zhu, Dongxu Liu, Peter E. Lobie
Jian‐Zhong Tang, Xiangjun Kong, Jian Jian Kang, Graeme C. Fielder, Michael Steiner, Jo K. Perry, Zhengsheng Wu, Zhinan Yin, Tao Zhu, Dongxu Liu, Peter E. Lobie
Nagarajan Kannan, Jian Jian Kang, Xiangjun Kong, Jian‐Zhong Tang, Jo K. Perry, Kumarasamypet M. Mohankumar, Lance D. Miller, Edison T. Liu, Hichem C. Mertani, Tao Zhu, Prudence M. Grandison, Dongxu Liu, Peter E. Lobie
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