化学
精氨酸
生物化学
甲基转移酶
酶
酶抑制剂
邻苯二酚-O-甲基转移酶
生物活性
酶激活剂
细胞培养
结构-活动关系
分子生物学
肽序列
赖氨酸
作者
Siqi Guo,Jianhao Li,Junjie Lin,Yan Chen,Chenyu Liu,H. Liu,Z. X. He,Yiyang Zhu,Lei Wang,Fan Yang,Cheng Luo,Zhihai Li,Jiamin Jin,Fei Ye
标识
DOI:10.1021/acs.jmedchem.5c03030
摘要
Protein arginine methyltransferase 1 (PRMT1) plays a critical role in cancer, yet current PRMT1 modulators lack selectivity and rely on enzymatic inhibition. Here, we developed first-in-class PRMT1-targeting PROTAC degrader compound 4, designed based on the pharmacophore of our previously developed PRMT1 inhibitor. Compound 4 potently induces PRMT1 degradation in a concentration-, time-, and proteasome-dependent manner and exhibits high selectivity, with no detectable degradation of other common CRBN substrates and other type I PRMTs. It also effectively inhibited the growth of multiple cancer cell lines and exhibited a favorable pharmacokinetic profile. Molecular modeling suggests that the unique conformation of the PRMT1 dimerization arm promotes productive ternary complex formation with CRBN, providing a structural basis for selective PRMT1 degradation. Overall, this study demonstrates that compound 4 is a first-in-class PRMT1-targeting PROTAC degrader and highlights its value as a chemical tool for studying PRMT1 biology and its therapeutic potential in PRMT1-dependent cancers.
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