In the present experiment, we find that UTI and TXT inhibit gene

In the present experiment, we find that UTI and TXT inhibit gene and protein expression check details of IGF-1R, PDGFA, NGF, NF-κB, and JNk-2 in breast carcinoma cells and the effect of UTI+TXT is strongest. In conclusion, this experiment demonstrates that

UTI and TXT inhibit proliferation of breast cancer cells and growth of xenografted breast tumors, induce apoptosis of breast cancer cells. UTI and TXT down-regulate the expression of mRNA and protein of IGF-1R, PDGFA, NGF, NF-κB, and JNk-2 in breast cancer cells and xenografted breast tumors. The effect of UTI+TXT is strongest. This suggests that UTI and TXT have synergistic effects. The mechanism might be related to a decrease in the signal transduction of JNk-2 and NF-κB, and then the expression of IGF-1R, PDGFA, NGF. Acknowledgements The project is supported by the Fund of Chongqing Science and Technology Commission (CSCT, this website 2008AC5082). References 1. Mohinta S, Mohinta H, Chaurasia P, Watabe K: Wnt pathway and breast cancer. Front Biosci 2007, 12:4020–4033.PubMedCrossRef 2. Takano H, Inoue K, Shimada A, Sato H, Yanagisawa Lenvatinib mouse R, Yoshikawa T: Urinary trypsin inhibitor protects against liver injury and coagulation pathway dysregulation induced by lipopolysaccharide/D-galactosamine in mice. Lab Invest 2009, 89:833–839.PubMedCrossRef 3. Inoue K, Takano H: Urinary trypsin inhibitor as a therapeutic option for endotoxin-related inflammatory disorders.

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