We describe a protein proximity inducing therapeutic modality called Regulated Induced Proximity Targeting Chimeras or RIPTACs: heterobifunctional small molecules that elicit a stable ternary complex between a target protein (TP) selectively expressed in tumor cells and a pan-expressed protein essential for cell survival. The resulting co-operative protein-protein interaction (PPI) abrogates the function of the essential protein, thus leading to death selectively in cells expressing the TP. This approach leverages differentially expressed intracellular proteins as novel cancer targets, with the advantage of not requiring the target to be a disease driver. In this chemical biology study, we design RIPTACs that incorporate a ligand against a model TP connected via a linker to effector ligands such as JQ1 (BRD4) or BI2536 (PLK1) or CDK inhibitors such as TMX3013 or dinaciclib. RIPTACs accumulate selectively in cells expressing the HaloTag-FKBP target, form co-operative intracellular ternary complexes, and induce an anti-proliferative response in target-expressing cells.
Regulated induced proximity targeting chimeras-RIPTACs-A heterobifunctional small molecule strategy for cancer selective therapies.
调控诱导邻近靶向嵌合体-RIPTACs-一种用于癌症选择性治疗的异双功能小分子策略
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作者:Raina Kanak, Forbes Chris D, Stronk Rebecca, Rappi Jonathan P Jr, Eastman Kyle J, Zaware Nilesh, Yu Xinheng, Li Hao, Bhardwaj Amit, Gerritz Samuel W, Forgione Mia, Hundt Abigail, King Madeline P, Posner Zoe M, Correia Allison D, McGovern Andrew, Puleo David E, Chenard Rebekka, Mousseau James J, Vergara J Ignacio, Garvin Ethan, Macaluso Jennifer, Martin Michael, Bassoli Kyle, Jones Kelli, Garcia Marco, Howard Katia, Yaggi Madeleine, Smith Levi M, Chen Jinshan M, Mayfield Andrew B, De Leon Cesar A, Hines John, Kayser-Bricker Katherine J, Crews Craig M
| 期刊: | Cell Chemical Biology | 影响因子: | 7.200 |
| 时间: | 2024 | 起止号: | 2024 Aug 15; 31(8):1490-1502 |
| doi: | 10.1016/j.chembiol.2024.07.005 | 研究方向: | 肿瘤 |
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