| Literature DB >> 30074276 |
Xiangdong Zhao1,2, Faliang Xu3, Nestor P Dominguez2,4, Yuanping Xiong2, Zhongxun Xiong3, Hong Peng1, Chloe Shay5,6, Yong Teng2,7.
Abstract
Although genetic amplification and overexpression of the fibroblast growth factor 19 (FGF19) gene are found in human breast cancer, mechanisms that contribute to such functional alterations remain elusive. We report here that high expression of FGF19 is associated with the aggressive malignant behavior and poor survival outcome of breast cancer patients. FGF19 is particularly highly expressed in luminal molecular subtype of breast tumors and its expression levels are positively associated with its secretion levels from breast cancer cells. Genetic knockout of FGF19 significantly induces repression of breast tumor progression and metastasis in either an orthotopic mouse model of breast cancer or an experimental metastasis model. The FGF19 specific receptor, FGFR4, can be activated and subsequently upregulate AKT signaling in breast cancer cell upon FGF19, which is critical for oncogenic role of FGF19. Inactivation of FGFR4 by its inhibitor BLU9931 significantly attenuates FGF19-induced tumor-promoting activity, suggesting interruption of FGFR4 function is sufficient to affect FGF19-driven breast cancer. Overall, these insights support the idea that targeting FGFR4 in breast cancer cells overexpressing FGF19 may represent an effective strategy to suppress cancer development, progression, and metastasis.Entities:
Keywords: AKT; BLU9931; FGF19; FGFR4; breast cancer; invasion and metastasis
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Year: 2018 PMID: 30074276 DOI: 10.1002/mc.22884
Source DB: PubMed Journal: Mol Carcinog ISSN: 0899-1987 Impact factor: 4.784