生物正交化学
化学
蛋白质降解
泛素连接酶
胞浆
生物化学
靶蛋白
蛋白质-蛋白质相互作用
体内
细胞生物学
泛素
声动力疗法
生物物理学
融合蛋白
膜蛋白
跨膜蛋白
蛋白质靶向
蛋白质工程
蛋白质生物合成
翻译(生物学)
转运蛋白
蛋白质稳定性
亚细胞定位
内化
点击化学
电穿孔
整体膜蛋白
细胞器
连接器
核糖体
内吞作用
作者
Yuhan Bao,Yaojin Zhu,Xinhao Wei,Yuxin Fang,Jiayi Zhu,Fei Gao,Guoqiang Dong,Shipeng He,Chunquan Sheng
标识
DOI:10.1002/advs.202520975
摘要
ABSTRACT Targeted protein degradation (TPD) offers powerful therapeutic opportunities but is limited by poor tissue penetration and E3 ligase dependence. Herein, we develop Sonodynamic Plug‐and‐Play Targeting Chimeras (SDPTAC), an ultrasound (US)‐activated, bioorthogonal strategy for in situ protein degradation. SDPTAC assembles via an inverse electron‐demand Diels–Alder (IEDDA) click reaction between a sonosensitizer and tetrazine‐tagged ligands, generating reactive oxygen species (ROS) upon US to degrade bound proteins. This modular platform enabled efficient degradation of nuclear (bromodomain‐containing protein 4, BRD4), cytosolic (nicotinamide phosphoribosyl transferase, NAMPT), and membrane (discoidin domain receptor 1, DDR1) targets, suppressed oncogenic signaling, and achieved nearly complete tumor growth inhibition in vivo with negligible toxicity. SDPTAC thus establishes a versatile, deep‐penetrating, and clinically translatable approach for noninvasive protein modulation.
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(2025-6-4)
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