A General Molecular Structural Design for Highly Efficient Photopyroptosis that can be Activated within 10 s Irradiation

Author:

Liu Qingsong123,Yao Xianxian1,Zhou Lulu1,Wu Wenfeng2,Cheng Jianshuo1,Zhang Zexin4,Li Zhongyu1,Sun Hao1,Jin Jian1,Zhang Man1,Wu Hongwei5,Zhu Shihui23ORCID,Yang Wuli1ORCID,Zhu Liangliang1ORCID

Affiliation:

1. State Key Laboratory of Molecular Engineering of Polymers Department of Macromolecular Science Fudan University Shanghai 200438 China

2. First Affiliated Hospital of Naval Military Medical University Shanghai 200438 China

3. Department of Burns and Plastic Surgery Shanghai Children's Medical Center School of Medicine Shanghai Jiao Tong University Shanghai 200127 China

4. Department of Burns and Plastic & Wound Repair Surgery Xiang'an Hospital of Xiamen University School of Medicine Xiamen University Xiamen 361102 China

5. College of Chemistry Chemical Engineering and Biotechnology Donghua University Shanghai 201620 China

Abstract

AbstractPhotopyroptosis is an emerging research branch of photodynamic therapy (PDT), whereas there remains a lack of molecular structural principles to fabricate photosensitizers for triggering a highly efficient pyroptosis. Herein, a general and rational structural design principle to implement this hypothesis, is proposed. The principle relies on the clamping of cationic moieties (e.g., pyridinium, imidazolium) onto one photosensitive core to facilitate a considerable mitochondrial targeting (both of the inner and the outer membranes) of the molecules, thus maximizing the photogenerated reactive oxygen species (ROS) at the specific site to trigger the gasdermin E‐mediated pyroptosis. Through this design, the pyroptotic trigger can be achieved in a minimum of 10 s of irradiation with a substantially low light dosage (0.4 J cm⁻2), compared to relevant work reported (up to 60 J cm⁻2). Moreover, immunotherapy with high tumor inhibition efficiency is realized by applying the synthetic molecules alone. This structural paradigm is valuable for deepening the understanding of PDT (especially the mitochondrial‐targeted PDT) from the perspective of pyroptosis, toward the future development of the state‐of‐the‐art form of PDT.

Funder

National Natural Science Foundation of China

Natural Science Foundation of Shanghai Municipality

Program of Shanghai Academic Research Leader

National Key Research and Development Program of China

Publisher

Wiley

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