鸦胆子素D通过靶向β-连环蛋白/锯齿蛋白1信号通路抑制肝癌生长。

Bruceine D inhibits hepatocellular carcinoma growth by targeting β-catenin/jagged1 pathways.

作者信息

Cheng Ziying, Yuan Xing, Qu Yi, Li Xia, Wu Guozhen, Li Chenwei, Zu Xianpeng, Yang Niao, Ke Xisong, Zhou Juan, Xie Ning, Xu Xike, Liu Shanrong, Shen Yunheng, Li Huiliang, Zhang Weidong

机构信息

Department of Phytochemistry, School of Pharmacy, Second Military Medical University, Shanghai 200433, China.

Interdisciplinary Science Research Institute, Shanghai University of Traditional Chinese Medicine, Shanghai 201203, PR China.

出版信息

Cancer Lett. 2017 Sep 10;403:195-205. doi: 10.1016/j.canlet.2017.06.014. Epub 2017 Jun 20.

DOI:10.1016/j.canlet.2017.06.014

PMID:28645563

Abstract

Hepatocellular carcinoma (HCC) is known for high mortality and limited available treatments. Aberrant activation of the Wnt and Notch signaling pathways is critical to liver carcinogenesis and progression. Here, we identified a small molecule, bruceine D (BD), as a Notch inhibitor, using an RBP-Jκ-dependent luciferase-reporter system. BD significantly inhibited liver tumor growth and enhanced the therapeutic effects of sorafenib in various murine HCC models. Mechanistically, BD promotes proteasomal degradation of β-catenin and the depletion of its nuclear accumulation, which in turn disrupts the Wnt/β-catenin-dependent transcription of the Notch ligand Jagged1 in HCC. Our findings provide important information about a novel Wnt/Notch crosstalk inhibitor that is synergistic with sorafenib for treatment of HCC, and therefore have high clinical impact.

摘要

肝细胞癌（HCC）以高死亡率和有限的可用治疗方法而闻名。Wnt和Notch信号通路的异常激活对肝癌的发生和发展至关重要。在这里，我们使用RBP-Jκ依赖性荧光素酶报告系统鉴定出一种小分子——鸦胆子素D（BD）作为Notch抑制剂。在各种小鼠肝癌模型中，BD显著抑制肝肿瘤生长并增强索拉非尼的治疗效果。从机制上讲，BD促进β-连环蛋白的蛋白酶体降解并减少其核积累，进而破坏肝癌中Notch配体Jagged1的Wnt/β-连环蛋白依赖性转录。我们的研究结果提供了关于一种新型Wnt/Notch串扰抑制剂的重要信息，该抑制剂与索拉非尼协同治疗肝癌，因此具有很高的临床意义。

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Bruceine D inhibits hepatocellular carcinoma growth by targeting β-catenin/jagged1 pathways.鸦胆子素D通过靶向β-连环蛋白/锯齿蛋白1信号通路抑制肝癌生长。

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鸦胆子素D通过靶向β-连环蛋白/锯齿蛋白1信号通路抑制肝癌生长。

Bruceine D inhibits hepatocellular carcinoma growth by targeting β-catenin/jagged1 pathways.

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