Enhancement strategy for effective vascular regeneration following myocardial infarction through a dual stem cell approach

Author:

Kim HyeokORCID,Park Soon-Jung,Park Jae-Hyun,Lee Sunghun,Park Bong-Woo,Lee Soon Min,Hwang Ji-Won,Kim Jin-Ju,Kang Byeongmin,Sim Woo-Sup,Kim Hyo-Jin,Jeon Seung Hwan,Kim Dong-Bin,Jang Jinah,Cho Dong-WooORCID,Moon Sung-Hwan,Park Hun-JunORCID,Ban Kiwon

Abstract

AbstractSince an impaired coronary blood supply following myocardial infarction (MI) negatively affects heart function, therapeutic neovascularization is considered one of the major therapeutic strategies for cell-based cardiac repair. Here, to more effectively achieve therapeutic neovascularization in ischemic hearts, we developed a dual stem cell approach for effective vascular regeneration by utilizing two distinct types of stem cells, CD31+-endothelial cells derived from human induced pluripotent stem cells (hiPSC-ECs) and engineered human mesenchymal stem cells that continuously secrete stromal derived factor-1α (SDF-eMSCs), to simultaneously promote natal vasculogenesis and angiogenesis, two core mechanisms of neovascularization. To induce more comprehensive vascular regeneration, we intramyocardially injected hiPSC-ECs to produce de novo vessels, possibly via vasculogenesis, and a 3D cardiac patch encapsulating SDF-eMSCs (SDF-eMSC-PA) to enhance angiogenesis through prolonged secretion of paracrine factors, including SDF-1α, was implanted into the epicardium of ischemic hearts. We verified that hiPSC-ECs directly contribute to de novo vessel formation in ischemic hearts, resulting in enhanced cardiac function. In addition, the concomitant implantation of SDF1α-eMSC-PAs substantially improved the survival, retention, and vasculogenic potential of hiPSC-ECs, ultimately achieving more comprehensive neovascularization in the MI hearts. Of note, the newly formed vessels through the dual stem cell approach were significantly larger and more functional than those formed by hiPSC-ECs alone. In conclusion, these results provide compelling evidence that our strategy for effective vascular regeneration can be an effective means to treat ischemic heart disease.

Funder

Research Grants Council, University Grants Committee

Ministry of Trade, Industry and Energy

Ministry of Health and Welfare

Ministry of Food and Drug Safety

National Research Foundation of Korea

Publisher

Springer Science and Business Media LLC

Subject

Clinical Biochemistry,Molecular Biology,Molecular Medicine,Biochemistry

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