Antioxidant Nanozyme‐Engineered Mesenchymal Stem Cells for In Vivo MRI Tracking and Synergistic Therapy of Myocardial Infarction

Author:

Le Wenjun12ORCID,Sun Zeyi1,Li Tieyan3,Cao Hao3,Yang Chuanxue1,Mei Tianxiao1,Zhang Laihai1,Wang Yibing4,Jia Wenwen2,Sun Wen5ORCID,Hu Yihui1,Liu Zhongmin123

Affiliation:

1. Institute for Regenerative Medicine Shanghai East Hospital School of Medicine Tongji University Shanghai 200092 China

2. Shanghai Institute of Stem Cell Research and Clinical Translation Shanghai 200120 China

3. Department of Cardiovascular Surgery Shanghai Heart Failure Research Center Shanghai East Hospital School of Medicine Tongji University Shanghai 200092 China

4. Department of Radiology Shanghai East Hospital School of Medicine Tongji University Shanghai 200092 China

5. State Key Laboratory of Fine Chemicals Frontiers Science Center for Smart Materials Oriented Chemical Engineering Dalian University of Technology Dalian 116024 China

Abstract

AbstractCell therapy is a promising approach for myocardial infarction (MI) treatment. However, this strategy is often restricted by the harsh microenvironment of MI, such as excess ROS, high oxidative stress, inflammation, etc., and thus decreases the curative effect. Additionally, the distribution, migration, and homing of the transplanted stem cells is ambiguous, which also becomes a bottleneck for clinical translation. To address these challenges, herein, a versatile antioxidant nanozyme is designed by polymerically modifying dopamine (PDA) onto the surface of Mn3O4. The obtained nanozyme acts as an efficient SOD mimic, eliminating ROS, relieving oxidative stress, and reducing inflammation to improve the MI microenvironment. Simultaneously, Mn3O4@PDA serves as an excellent MRI contrast agent for tracking MSCs. Then, MSCs are engineered with Mn3O4@PDA nanozyme via endocytosis to form Mn3O4@PDA‐MSCs (Abbr. E‐MSCs), which possess superior viability, migration and homing ability compared to normal MSCs. Furthermore, E‐MSCs exhibit superior anti‐oxidant and anti‐inflammatory activity, thereby enhancing the therapeutic efficacy of MSCs. Finally, the in vivo MRI tracking and synergistic therapy potential of E‐MSCs is explored in MI model mice. Overall, this work provides a strategy to combine antioxidant activity and imaging properties of nanozymes to simultaneously facilitate imaging tracking of stem cells and improve MI treatment.

Funder

National Natural Science Foundation of China

Shanghai Municipal Health Commission

Publisher

Wiley

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