Erythrocyte Membrane Camouflaged Nanotheranostics for Optical Molecular Imaging‐Escorted Self‐Oxygenation Photodynamic Therapy

Author:

Wan Yilin12,Li Chunying2,Fu Lian‐Hua2,Feng Ting1,Zhang Yifan2,Li Youyan2,Lin Jing2,Huang Peng2ORCID,Cui Da‐Xiang1

Affiliation:

1. Institute of Nano Biomedicine and Engineering Shanghai Engineering Research Center for Intelligent Diagnosis and Treatment Instrument School of Sensing Science and Engineering School of Electronic Information and Electrical Engineering Shanghai Jiao Tong University 800 Dongchuan Road Shanghai 200240 China

2. Marshall Laboratory of Biomedical Engineering International Cancer Center Laboratory of Evolutionary Theranostics (LET) School of Biomedical Engineering Shenzhen University Medical School Shenzhen University Shenzhen 518055 China

Abstract

AbstractHypoxic tumor microenvironment (TME) hampers the application of oxygen (O2)‐dependent photodynamic therapy (PDT) in solid tumors. To address this problem, a biomimetic nanotheranostics (named MMCC@EM) is developed for optical molecular imaging‐escorted self‐oxygenation PDT. MMCC@EM is synthesized by encapsulating chlorin e6 (Ce6) and catalase (CAT) in metal–organic framework (MOF) nanoparticles with erythrocyte membrane (EM) camouflage. Based on the biomimetic properties of EM, MMCC@EM efficiently accumulates in tumor tissues. The enriched MMCC@EM achieves TME‐activatable drug release, thereby releasing CAT and Ce6, and this process can be monitored through fluorescence (FL) imaging. In addition, endogenous hydrogen peroxide (H2O2) will be decomposed by CAT to produce O2, which can be reflected by the measurement of intratumoral oxygen concentration using photoacoustic (PA) imaging. Such self‐oxygenation nanotheranostics effectively mitigate tumor hypoxia and improve the generation of singlet oxygen (1O2). The 1O2 disrupts mitochondrial function and triggers caspase‐3‐mediated cellular apoptosis. Furthermore, MMCC@EM triggers immunogenic cell death (ICD) effect, leading to an increased infiltration of cytotoxic T lymphocytes (CTLs) into tumor tissues. As a result, MMCC@EM exhibits good therapeutic effects in 4T1‐tumor bearing mice under the navigation of FL/PA duplex imaging.

Funder

National Key Research and Development Program of China

National Natural Science Foundation of China

Publisher

Wiley

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