Integration of Activation by Hypoxia and Inhibition Resistance of Tumor Cells to Apoptosis for Precise and Augmented Photodynamic Therapy

Author:

Shao Yutong1,Chen Miaomiao12,Chen Wenlong2,Wang Zehui2,Sui Mengzhang2,Tian Mingyu2,Wu Yingnan1,Song Jitao1,Ji Debin1,Song Fengling12ORCID

Affiliation:

1. Institute of Molecular Sciences and Engineering Institute of Frontier and Interdisciplinary Science Shandong University Qingdao 266237 P. R. China

2. State Key Laboratory of Fine Chemicals School of Chemical Engineering Dalian University of Technology Dalian 116024 P. R. China

Abstract

AbstractPhotodynamic therapy (PDT) uses photosensitizers to convert oxygen (O2) to reactive oxygen species (ROS) under irradiation to induce DNA damage and kill cancer cells. However, the effect of PDT is usually alleviated by apoptosis resistance mechanism of tumor living cells. MTH1 enzyme is known to be such an apoptosis‐resistance enzyme which is over expressed as a scavenger to repair the damaged DNA. In this work, a hypoxia‐activated nanosystem FTPA, which can be degraded to release the encapsulated PDT photosensitizer 4‐DCF‐MPYM and an inhibitor TH588 is proposed. The inhibitor TH588 can inhibit the DNA repair process by reducing the activity of MTH1 enzyme, and achieve the purpose of amplifying the therapeutic effect of PDT. This work demonstrates that a precise and augmented tumor PDT is achieved by integration of hypoxia‐activation and inhibition resistance of tumor cells to apoptosis.

Funder

National Natural Science Foundation of China

Fundamental Research Funds for the Central Universities

Publisher

Wiley

Subject

Pharmaceutical Science,Biomedical Engineering,Biomaterials

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