Chen Kuen-Feng, Tai Wei-Tien, Huang Jui-Wen, Hsu Cheng-Yi, Chen Wei-Lin, Cheng Ann-Lii, Chen Pei-Jer, Shiau Chung-Wai
Department of Medical Research, National Taiwan University Hospital, 7, Chung-Shan South Road, Taipei, Taiwan, Republic of China.
Eur J Med Chem. 2011 Jul;46(7):2845-51. doi: 10.1016/j.ejmech.2011.04.007. Epub 2011 Apr 14.
STAT3 is a transcription factor that modulates survival-directed transcription. It is persistently activated in many human cancers. Literature has shown that sorafenib, Raf kinase inhibitor, reduces Phospho-STAT3 and induces cell death. A series of sorafenib derivatives were synthesized as new inhibitors for STAT3. Urea, sulfonamide, and carboxamide linkers brought out different SARs from the end of sorafenib. Urea and carboxamide linked derivatives showed greater inhibition against STAT3 activity than sulfonamide linked derivatives. In particular, 1-(4-chloro-3-(trifluoromethyl)phenyl)-3-(4-(4-cyanophenoxy)phenyl)urea (1), a urea linker, was as potent as sorafenib in reducing P-STAT3 level and cell death but no inhibition for Raf activity. Such result provides a new lead for the design of STAT3 inhibitors.
信号转导子和转录激活子3(STAT3)是一种调节生存导向转录的转录因子。它在许多人类癌症中持续激活。文献表明,Raf激酶抑制剂索拉非尼可降低磷酸化STAT3水平并诱导细胞死亡。合成了一系列索拉非尼衍生物作为STAT3的新型抑制剂。脲、磺酰胺和羧酰胺连接基从索拉非尼末端产生了不同的构效关系。脲和羧酰胺连接的衍生物对STAT3活性的抑制作用比磺酰胺连接的衍生物更强。特别是,脲连接的1-(4-氯-3-(三氟甲基)phenyl)-3-(4-(4-氰基苯氧基)phenyl)脲(1)在降低磷酸化STAT3水平和诱导细胞死亡方面与索拉非尼一样有效,但对Raf活性无抑制作用。该结果为STAT3抑制剂的设计提供了新的先导化合物。
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