Structure-Based Discovery of Selective Histone Deacetylase 8 Degraders with Potent Anticancer Activity.
Jinbo HuangJun ZhangWenchao XuQiong WuRongsheng ZengZhichao LiuWenhui TaoQian ChenYongqing WangWei-Guo ZhuPublished in: Journal of medicinal chemistry (2022)
Inducing protein degradation by proteolysis targeting chimeras has gained tremendous momentum as a promising novel therapeutic strategy. Here, we report the design, synthesis, and biological characterization of highly potent proteolysis targeting chimeric small molecules targeting the epigenetic regulator histone deacetylase 8 (HDAC8). We developed potent and effective HDAC8 degraders, as exemplified by SZUH280 ( 16e ), which effectively induced HDAC8 protein degradation and inhibited cancer cell growth even at low micromolar concentrations. Our preliminary mechanistic studies revealed that SZUH280 hampers DNA damage repair in cancer cells, promoting cellular radiosensitization. In mice, a single SZUH280 dose induced rapid and prolonged HDAC8 protein degradation in xenograft tumor tissues. Moreover, SZUH280 alone or in combination with irradiation resulted in long-lasting tumor regression in an A549 tumor mouse model. Our findings qualify a new chemical tool for HDAC8 knockdown and may lead to the development of a new class of cancer therapeutics.
Keyphrases
- histone deacetylase
- dna damage
- papillary thyroid
- mouse model
- protein protein
- small molecule
- high glucose
- gene expression
- diabetic rats
- oxidative stress
- squamous cell
- amino acid
- binding protein
- cell therapy
- anti inflammatory
- stem cells
- childhood cancer
- single cell
- transcription factor
- high throughput
- drug induced
- endothelial cells
- dna repair
- young adults
- skeletal muscle
- case control