Radiotherapy-Induced Cleavage of Quaternary Ammonium Groups Activates Prodrugs in Tumors.
Zhibin GuoHanyu HongYuedan ZhengZiyang WangZexuan DingQunfeng FuZhibo LiuPublished in: Angewandte Chemie (International ed. in English) (2022)
Cleavage chemistry offers a new chance to activate chemotherapeutic prodrugs in a tumor-selective manner, yet developing spatiotemporally controllable cleavage chemistry with deep tissue penetration is still a great challenge. Herein, we present a novel radiotherapy-triggered cleavage chemistry that enables controlled drug release in tumors. Quaternary ammonium groups are identified as masking groups that can be efficiently removed by hydrated electrons (e - aq ) from water radiolysis. The subsequently released tertiary amines can be anti-cancer toxins or readily release functional molecules via 1,6-elimination. This radiotherapy-induced cleavage works successfully in living cells and tumor-bearing mice, showing remarkable treatment efficacy when the mice are given carfilzomib prodrug and radiotherapy. This strategy provides a new perspective for combinational radiochemotherapy, which is the first-line treatment for over 50 % of cancer patients.
Keyphrases
- locally advanced
- early stage
- drug release
- dna binding
- living cells
- radiation therapy
- radiation induced
- high glucose
- fluorescent probe
- rectal cancer
- diabetic rats
- squamous cell carcinoma
- drug delivery
- drug discovery
- high fat diet induced
- drug induced
- transcription factor
- ionic liquid
- type diabetes
- single molecule
- multiple myeloma
- cancer therapy
- smoking cessation