生物正交化学
癌症治疗
癌症研究
BRD4
化学
靶向治疗
三元络合物
癌症
蛋白质降解
计算生物学
机制(生物学)
端粒酶
泛素
药物发现
癌症治疗
靶蛋白
表观遗传学
溴尿嘧啶
癌细胞
细胞生物学
纳米技术
作者
Yanyun Hong,Xiang Liu,Yanfang Li,Mengting Yu,Caolin Wang,Cunpeng Nie,Shan Xu
摘要
the ubiquitin-proteasome system (UPS). This review systematically summarizes developments over the past decade in BRD4-targeting PROTACs for cancer therapy, focusing on ternary complex design optimization, bioorthogonal activation strategies, and innovations in delivery systems. PROTACs facilitate BRD4 ubiquitination and degradation by simultaneously recruiting BRD4 and various E3 ligases, including CRBN, VHL, MDM2, and DCAF. By integrating BRD4 ligands (JQ1, ABBV-075, and HJB97) with strategies like macrocyclization, dual-targeting designs, and the dTAG system, potency and isoform selectivity have been enhanced. To minimize off-target toxicity, bioorthogonal activation strategies-such as photocaging and chemically induced approaches-have been developed, alongside precision delivery systems like antibody-PROTACs, folate-PROTACs, and stimuli-responsive PROTACs. The novel mechanism of molecular glue degraders is also explored. Multidimensional optimization is now propelling BRD4-PROTACs towards clinical translation, promising efficient, safe, and precisely controllable new strategies for cancer treatment.
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