1. A potent and selective small molecule inhibitor ofmyoferlin attenuates colorectal cancer progression.
- Author
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Yuan He, Weiqiong Kan, Yunqi Li, Yun Hao, Anling Huang, Haijun Gu, Minna Wang, Qingqing Wang, Jinlian Chen, Zhenliang Sun, Mingyao Liu, Yihua Chen, and Zhengfang Yi
- Subjects
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COLORECTAL cancer , *SMALL molecules , *CANCER invasiveness - Abstract
As a pivotal vesicular trafficking protein, Myoferlin (MYOF) has become an attractive target for cancer therapy.However, the roles ofMYOF in colorectal cancer invasion remain enigmatic, and MYOF-targeted therapy in this malignancy has not been explored. In the present study, we provided the first functional evidence that MYOF promoted the cell invasion of colorectal cancer. Furthermore, we identified a novel small molecule inhibitor of MYOF (named YQ456) that showed high binding affinity toMYOF (KD = 37 nM) and excellent anti-invasion capability (IC50 = 110 nM). YQ456 was reported for the first time to interfere with the interactions between MYOF and Ras-associated binding (Rab) proteins at low nanomolar levels. This interference disrupted several vesicle trafficking processes, including lysosomal degradation, exosome secretion, and mitochondrial dynamics. Further, YQ456 exhibited excellent inhibitory effects on the growth and invasiveness of colorectal cancer. As the first attempt, the anticancer efficacy of YQ456 in the patient-derived xenograft (PDX) mouse model indicated that targeting MYOF may serve as a novel and practical therapeutic approach for colorectal cancer. [ABSTRACT FROM AUTHOR]
- Published
- 2021
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