Metal protoporphyrin‐induced self‐assembly nanoprobe enabling precise tracking and antioxidant protection of stem cells for ischemic stroke therapy

Author:

Shu Yimeng12,Shen Hui3,Yao Minghua4,Shen Jie12,Yang Guo‐Yuan3,Chen Hangrong125,Tang Yaohui36,Ma Ming125ORCID

Affiliation:

1. State Key Laboratory of High Performance Ceramics and Superfine Microstructures Shanghai Institute of Ceramics Chinese Academy of Sciences Shanghai China

2. Center of Materials Science and Optoelectronics Engineering University of Chinese Academy of Sciences Beijing China

3. Med‐X Research Institute and School of Biomedical Engineering Shanghai Jiao Tong University Shanghai China

4. Department of Ultrasound Shanghai General Hospital School of Medicine Shanghai Jiao Tong University Shanghai China

5. School of Chemistry and Materials Science Hangzhou Institute for Advanced Study University of Chinese Academy of Sciences Hangzhou China

6. Ankerui (Shanxi) Biological Cell Co., Ltd. Xiaohe Industrial Park Comprehensive Reform Demonstration Zone Taiyuan China

Abstract

AbstractMesenchymal stem cell (MSC)‐based therapy has provided a promising strategy for the treatment of ischemic stroke, which is still restricted by the lack of long‐term cell tracking strategy as well as the poor survival rate of stem cells in ischemic region. Herein, a dual‐functional nanoprobe, cobalt protoporphyrin‐induced nano‐self‐assembly (CPSP), has been developed through a cobalt protoporphyrin IX (CoPP) aggregation‐induced self‐assembly strategy, which combines CoPP and superparamagnetic iron oxide (SPION) via a simple solvent evaporation‐driven method. Without any additional carrier materials, the obtained CPSP is featured with good biocompatibility and high proportions of active ingredients. The SPIONs in CPSPs form a cluster‐like structure, endowing this nano‐self‐assembly with excellent T2‐weighted magnetic resonance (MR) imaging performance. Furthermore, the CoPP released from CPSPs could effectively protect MSCs by upregulating heme oxygenase 1 (HO‐1) expression. The in vivo cell tracing capacity of CPSPs is confirmed by monitoring the migration of labeled MSCs with MR imaging in a middle cerebral artery occlusion mouse model. More importantly, the sustained release of CoPP from CPSPs improves the survival of transplanted MSCs and promotes neural repair and neurobehavioral recovery of ischemic mice. Overall, this work presents a novel dual‐functional nanoagent with an ingenious design for advancing MSC‐based therapy.

Publisher

Wiley

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