Copper(II) complex enhanced chemodynamic therapy through GSH depletion and autophagy flow blockade.
Wen-Ying ShenChun-Peng JiaLi-Yi LiaoLiu-Lin ChenCheng-Cheng YuanYun-Qiong GuYang-Han LiuHong LiangZhen-Feng ChenPublished in: Dalton transactions (Cambridge, England : 2003) (2023)
Three copper(II) complexes C1-C3 were synthesized and fully characterized as chemodynamic therapy (CDT) anticancer agents. C1-C3 showed greater cytotoxicity than their ligands toward SK-OV-3 and T24 cells. Particularly, C2 showed high cytotoxicity toward T24 cells and low cytotoxicity toward normal human HL-7702 and WI-38 cells. Mechanistic studies demonstrated that C2 oxidized GSH to GSSG and produced ˙OH, which induced mitochondrial dysfunction and ER stress, finally leading to apoptosis of T24 cells. In addition, C2 inhibited autophagy by blocking autophagy flow, thereby closing the self-protection pathway of oxidative stress to enhance CDT. Importantly, C2 significantly inhibited T24 tumor growth with 57.1% inhibition in a mouse xenograft model. C2 is a promising lead as a potential CDT anticancer agent.
Keyphrases
- oxidative stress
- induced apoptosis
- endoplasmic reticulum stress
- cell death
- cell cycle arrest
- diabetic rats
- signaling pathway
- endothelial cells
- dna damage
- ischemia reperfusion injury
- oxide nanoparticles
- high glucose
- fluorescent probe
- mesenchymal stem cells
- risk assessment
- human health
- low density lipoprotein
- cell therapy