Dual‐Responsive Turn‐On T1 Imaging‐Guided Mild Photothermia for Precise Apoptotic Cancer Therapy

Author:

Song Sijie1,Wang Qi1,Xie Jiangao2,Dai Junduan1,Ouyang Dilan1,Huang Guoming3,Guo Yuheng1,Chen Chen1,Wu Mengnan1,Huang Tingjing1,Ruan Jingwen1,Cheng Xiaofeng1,Lin Xucong4,He Yu1,Rozhkova Elena A.5ORCID,Chen Zhaowei1ORCID,Yang Huanghao1ORCID

Affiliation:

1. MOE Key Laboratory for Analytical Science of Food Safety and Biology, Fujian Provincial Key Laboratory of Analysis and Detection Technology for Food Safety, and State Key Laboratory of Photocatalysis on Energy and Environment, College of Chemistry Fuzhou University Fuzhou 350108 P. R. China

2. Fujian Medical University Union Hospital Fuzhou 350108 P. R. China

3. College of Biological Science and Engineering Fuzhou University Fuzhou 350108 P. R. China

4. Engineering Technology Research Center on Reagent and Instrument for Rapid Detection of Product Quality and Food Safety in Fujian Province, College of Chemistry Fuzhou University Fuzhou 350108 P. R. China

5. Center for Nanoscale Materials Argonne National Laboratory Argonne IL 60439 USA

Abstract

AbstractApoptosis has gained increasing attention in cancer therapy as an intrinsic signaling pathway, which leads to minimal leakage of waste products from a dying cell to neighboring normal cells. Among various stimuli to trigger apoptosis, mild hyperthermia is attractive but confronts limitations of non‐specific heating and acquired resistance from elevated expression of heat shock proteins. Here, a dual‐stimulation activated turn‐on T1 imaging‐based nanoparticulate system (DAS) is developed for mild photothermia (≈43 °C)‐mediated precise apoptotic cancer therapy. In the DAS, a superparamagnetic quencher (ferroferric oxide nanoparticles, Fe3O4 NPs) and a paramagnetic enhancer (Gd‐DOTA complexes) are connected via the N6‐methyladenine (m6A)‐caged, Zn2+‐dependent DNAzyme molecular device. The substrate strand of the DNAzyme contains one segment of Gd‐DOTA complex‐labeled sequence and another one of HSP70 antisense oligonucleotide. When the DAS is taken up by cancer cells, overexpressed fat mass and obesity‐associated protein (FTO) specifically demethylates the m6A group, thereby activating DNAzymes to cleave the substrate strand and simultaneously releasing Gd‐DOTA complex‐labeled oligonucleotides. The restored T1 signal from the liberated Gd‐DOTA complexes lights up the tumor to guide the location and time of deploying 808 nm laser irradiation. Afterward, locally generated mild photothermia works in concert with HSP70 antisense oligonucleotides to promote apoptosis of tumor cells. This highly integrated design provides an alternative strategy for mild hyperthermia‐mediated precise apoptotic cancer therapy.

Funder

National Key Research and Development Program of China

National Natural Science Foundation of China

Basic Energy Sciences

Publisher

Wiley

Subject

Pharmaceutical Science,Biomedical Engineering,Biomaterials

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