Near-Infrared Light-Initiated Molecular Superoxide Radical Generator: Rejuvenating Photodynamic Therapy against Hypoxic Tumors

Mingle Li(Dalian University of Technology), Jing Xia(Dalian University of Technology), Ruisong Tian(Dalian University of Technology), Jingyun Wang(Dalian University of Technology), Jiangli Fan(Dalian University of Technology), Jianjun Du(Dalian University of Technology), Saran Long(Dalian University of Technology), Xiangzhi Song(Central South University), James W. Foley(Harvard University Press), Xiaojun Peng(Dalian University of Technology)
Journal of the American Chemical Society
October 17, 2018
Cited by 654

Abstract

Hypoxia, a quite universal feature in most solid tumors, has been considered as the “Achilles’ heel” of traditional photodynamic therapy (PDT) and substantially impairs the overall therapeutic efficacy. Herein, we develop a near-infrared (NIR) light-triggered molecular superoxide radical (O2–•) generator (ENBS-B) to surmount this intractable issue, also reveal its detailed O2–• action mechanism underlying the antihypoxia effects, and confirm its application for in vivo targeted hypoxic solid tumor ablation. Photomediated radical generation mechanism study shows that, even under severe hypoxic environment (2% O2), ENBS-B can generate considerable O2–• through type I photoreactions, and partial O2–• is transformed to high toxic OH· through SOD-mediated cascade reactions. These radicals synergistically damage the intracellular lysosomes, which subsequently trigger cancer cell apoptosis, presenting a robust hypoxic PDT potency. In vitro coculture model shows that, benefiting from biotin ligand, ENBS-B achieves 87-fold higher cellular uptake in cancer cells than normal cells, offering opportunities for personalized medicine. Following intravenous administration, ENBS-B is able to specifically target to neoplastic tissues and completely suppresses the tumor growth at a low light-dose irradiation. As such, we postulated this work will extend the options of excellent agents for clinical cancer therapy.


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