TF-PROTACs Enable Targeted Degradation of Transcription Factors

泛素连接酶 转录因子 化学 蛋白酶体 泛素 计算生物学 蛋白质降解 寡核苷酸 蛋白质水解 DNA 细胞生物学 生物 生物化学 基因
作者
Jing Liu,He Chen,H. Ümit Kanıskan,Ling Xie,Xian Chen,Jian Jin,Wenyi Wei
出处
期刊:Journal of the American Chemical Society [American Chemical Society]
卷期号:143 (23): 8902-8910 被引量:171
标识
DOI:10.1021/jacs.1c03852
摘要

Transcription factors (TFs) represent a major class of therapeutic targets for the treatment of human diseases including cancer. Although the biological functions and even crystal structures of many TFs have been clearly elucidated, there is still no viable approach to target the majority of TFs, thus rendering them undruggable for decades. PROTACs (proteolysis targeting chimeras) emerge as a powerful class of therapeutic modalities, which rely on induced protein–protein interactions between the proteins of interest (POIs) and E3 ubiquitin ligases to aid the degradation of POIs by the ubiquitin-proteasome system (UPS). Here, we report the development of a platform termed TF-PROTAC, which links an DNA oligonucleotide to an E3 ligase ligand via a click reaction, to selectively degrade the TF of interest. The selectivity of these TF-PROTACs depends on the DNA oligonucleotides utilized that can be specific to the TFs of interest. We have developed two series of VHL-based TF-PROTACs, NF-κB-PROTAC (dNF-κB) and E2F-PROTAC (dE2F), which effectively degrade endogenous p65 and E2F1 proteins in cells, respectively, and subsequently display superior antiproliferative effects in cells. Collectively, our results suggest that TF-PROTACs provide a generalizable platform to achieve selective degradation of TFs and a universal strategy for targeting most "undruggable" TFs.
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