大肠腺瘤性息肉病
拟肽
结直肠癌
CDC42型
癌症研究
癌症
癌细胞
细胞生物学
生物
医学
信号转导
生物化学
内科学
肽
作者
Haiming Jiang,Rong Deng,Xiuyan Yang,Jialin Shang,Shaoyong Lu,Yanlong Zhao,Kun Song,Xinyi Liu,Qiufen Zhang,Yu Chen,Y. Eugene Chinn,Geng Wu,Jian Li,Guoqiang Chen,Jianxiu Yu,Jian Zhang
标识
DOI:10.1038/nchembio.2442
摘要
The binding of adenomatous polyposis coli (APC) to its receptor Asef relieves the negative intramolecular regulation of Asef and leads to aberrant cell migration in human colorectal cancer. Because of its crucial role in metastatic dissemination, the interaction between APC and Asef is an attractive target for anti-colorectal-cancer therapy. We rationally designed a series of peptidomimetics that act as potent inhibitors of the APC interface. Crystal structures and biochemical and cellular assays showed that the peptidomimetics in the APC pocket inhibited the migration of colorectal cells by disrupting APC-Asef interaction. By using the peptidomimetic inhibitor as a chemical probe, we found that CDC42 was the downstream GTPase involved in APC-stimulated Asef activation in colorectal cancer cells. Our work demonstrates the feasibility of exploiting APC-Asef interaction to regulate the migration of colorectal cancer cells, and provides what to our knowledge is the first class of protein-protein interaction inhibitors available for the development of cancer therapeutics targeting APC-Asef signaling.
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