| Literature DB >> 34138566 |
Chaowei Ren1,2,3, Ning Sun1,4, Haixia Liu1,5,3, Ying Kong6, Renhong Sun1,4, Xing Qiu7, Jinju Chen6, Yan Li6, Jianshui Zhang6, Yuedong Zhou6, Hui Zhong1,8, Qianqian Yin1, Xiaoling Song1, Xiaobao Yang1, Biao Jiang1,5,7.
Abstract
Proteolysis-targeting chimera (PROTAC) is an attractive technology in drug discovery. Canonically, targets act as a basic starting point in the most previous PROTAC design. Here, we designed degraders considering from the view of clinical benefits. With this novel design, Brigatinib was turned into a degrader SIAIS164018 and endowed with unique features. First, SIAIS164018 could degrade not only ALK fusion proteins in activating or G1202R-mutated form but also mutant EGFR with L858R + T790M, which are two most important targets in non-small-cell lung cancer. Second, SIAIS164018 strongly inhibited cell migration and invasion of Calu-1 and MDA-MB-231. Third and surprisingly, SIAIS164018 degrades several important oncoproteins involved in metastasis such as FAK, PYK2, and PTK6. Interestingly, SIAIS164018 reshuffled the kinome ranking profile when compared to Brigatinib. Finally, SIAIS164018 is orally bioavailable and well tolerated in vivo. SIAIS164018 is an enlightening degrader for us to excavate the charm of protein degradation.Entities:
Year: 2021 PMID: 34138566 DOI: 10.1021/acs.jmedchem.1c00373
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446