An electro-ferroptotic nanoammunition enables image-guided, spatiotemporally controlled cancer ferroptosis induction via irreversible electroporation

Authors
Han, Jun-HyeokSeo, Hee SeungLee, JiyoungChen, ZhengWang, QiyueLee, Yun YoungLee, Na KyeongKang, Jeon MinKim, Song HeeHong, HwichanPark, Jung-HoonPiao, YuanzheLi, FangyuanNa, KunPark, Chun GwonPark, WooramLing, Daishun
Issue Date
2024-05
Publisher
Elsevier BV
Citation
Chemical Engineering Journal, v.487
Abstract
Ferroptosis, an iron -dependent regulated cell death pathway, has emerged as a promising modality for cancer therapy. However, current iron -based ferroptosis inducers, which trigger the Fenton reaction and release Fe2+, face challenges associated with limited cytosolic Fe2+ accumulation, leading to suboptimal ferroptosis induction. Herein, we report an electro-ferroptotic nanoammunition (EFN) composed of iron oxide nanoassembly (IONA) and ascorbic acid -loaded liposomes (Lip -AA) that enables image -guided, spatiotemporally controlled ferroptosis induction via irreversible electroporation (IRE) for enhanced cancer ferroptotic therapy. The IONA and Lip -AA form stable complexes through electrostatic interactions. Upon IRE stimulation, ascorbic acid is released from liposomes and reduce IONA to release abundant Fe2+. Moreover, IRE enhances tumor cell membrane permeability, thus facilitating efficient cytosolic Fe2+ accumulation for effective tumor ferroptosis. Notably, the Fe2+ release of EFN after IRE can be readily monitored by magnetic resonance imaging. Finally, IRE -triggered EFN demonstrates superior tumor growth inhibition, increased survival rates, and activation of immune cells, showing great potential for the development of next -generation spatiotemporally controlled ferroptotic therapies.
Keywords
THERMAL ABLATION; EFFICACY; Irreversible electroporation; Ferroptosis; Liposomes, Image-guided therapy; Cancer immunotherapy
ISSN
1385-8947
URI
https://pubs.kist.re.kr/handle/201004/149876
DOI
10.1016/j.cej.2024.150366
Appears in Collections:
KIST Article > 2024
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