Discovery of a new class of reversible TEA domain transcription factor inhibitors with a novel binding mode

被引:18
作者
Hu, Lu [1 ]
Sun, Yang [1 ]
Liu, Shun [2 ,3 ]
Erb, Hannah [1 ]
Singh, Alka [4 ]
Mao, Junhao [4 ]
Luo, Xuelian [2 ,3 ]
Wu, Xu [1 ]
机构
[1] Harvard Med Sch, Massachusetts Gen Hosp, Cutaneous Biol Res Ctr, Charlestown, MA 02115 USA
[2] Univ Texas Southwestern Med Ctr, Dept Pharmacol & Biophys, Dallas, TX 75390 USA
[3] Univ Texas Southwestern Med Ctr, Dept Biophys, Dallas, TX USA
[4] Univ Massachusetts, Med Sch, Dept Mol Cell & Canc Biol, Worcester, MA USA
来源
ELIFE | 2022年 / 11卷
关键词
medicinal chemistry; co-crytal structure; Hippo signaling; mouse; tead transcription factors; Human; HIPPO PATHWAY; EMERGING ROLES; YAP; PALMITOYLATION; YAP/TAZ; GROWTH; PROLIFERATION; OUTPUT;
D O I
10.7554/eLife.80210
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
The TEA domain (TEAD) transcription factor forms a transcription co-activation complex with the key downstream effector of the Hippo pathway, YAP/TAZ. TEAD-YAP controls the expression of Hippo-responsive genes involved in cell proliferation, development, and tumorigenesis. Hyperactivation of TEAD-YAP activities is observed in many human cancers and is associated with cancer cell proliferation, survival, and immune evasion. Therefore, targeting the TEAD-YAP complex has emerged as an attractive therapeutic approach. We previously reported that the mammalian TEAD transcription factors (TEAD1-4) possess auto-palmitoylation activities and contain an evolutionarily conserved palmitate-binding pocket (PBP), which allows small-molecule modulation. Since then, several reversible and irreversible inhibitors have been reported by binding to PBP. Here, we report a new class of TEAD inhibitors with a novel binding mode. Representative analog TM2 shows potent inhibition of TEAD auto-palmitoylation both in vitro and in cells. Surprisingly, the co-crystal structure of the human TEAD2 YAP-binding domain (YBD) in complex with TM2 reveals that TM2 adopts an unexpected binding mode by occupying not only the hydrophobic PBP, but also a new side binding pocket formed by hydrophilic residues. RNA-seq analysis shows that TM2 potently and specifically suppresses TEAD-YAP transcriptional activities. Consistently, TM2 exhibits strong antiproliferation effects as a single agent or in combination with a MEK inhibitor in YAP-dependent cancer cells. These findings establish TM2 as a promising small-molecule inhibitor against TEAD-YAP activities and provide new insights for designing novel TEAD inhibitors with enhanced selectivity and potency.
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页数:22
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