Oct4-dependent FoxC1 activation improves the survival and neovascularization of mesenchymal stem cells under myocardial ischemia

Zhou Ji; Songsheng Chen; Jin Cui; Weiguang Huang; Rui Zhang; Jianrui Wei; Shaoheng Zhang

doi:10.1186/s13287-021-02553-w

Oct4-dependent FoxC1 activation improves the survival and neovascularization of mesenchymal stem cells under myocardial ischemia

Stem Cell Res Ther. 2021 Aug 28;12(1):483. doi: 10.1186/s13287-021-02553-w.

Authors

Zhou Ji^#^{1

2}, Songsheng Chen^#¹, Jin Cui¹, Weiguang Huang¹, Rui Zhang¹, Jianrui Wei¹, Shaoheng Zhang³

Affiliations

¹ Department of Cardiology, Guangzhou Red Cross Hospital Medical College of Jinan University, 396 Tongfuzhong Road, Haizhu District, Guangzhou, 510220, China.
² Department of Cardiology, The Third Affiliated Hospital of Jinzhou Medical University, Jinzhou, 121001, Liaoning, China.
³ Department of Cardiology, Guangzhou Red Cross Hospital Medical College of Jinan University, 396 Tongfuzhong Road, Haizhu District, Guangzhou, 510220, China. shaohengzhang67@163.com.

^# Contributed equally.

Abstract

Background: The administration of mesenchymal stem cells (MSCs) remains the most promising approach for cardiac repair after myocardial infarct (MI). However, their poor survival and potential in the ischemic environment limit their therapeutic efficacy for heart repair after MI. The purpose of this study was to investigate the influence of FoxC1-induced vascular niche on the activation of octamer-binding protein 4 (Oct4) and the fate of MSCs under hypoxic/ischemic conditions.

Methods: Vascular microenvironment/niche was induced by efficient delivery of FoxC1 transfection into hypoxic endothelial cells (ECs) or infarcted hearts. MSCs were cultured or injected into this niche by utilizing an in vitro coculture model and a rat MI model. Survival and neovascularization of MSCs regulated by Oct4 were explored using gene transfer and functional studies.

Results: Here, using gene expression heatmap, we demonstrated that cardiac ECs rapidly upregulated FoxC1 after acute ischemic cardiac injury, contributing to an intrinsic angiogenesis. In vitro, FoxC1 accelerated tube-like structure formation and increased survival of ECs, resulting in inducing a vascular microenvironment. Overexpression of FoxC1 in ECs promoted survival and neovascularization of MSCs under hypoxic coculture. Overexpression of Oct4, a FoxC1 target gene, in MSCs enhanced their mesenchymal-to-endothelial transition (MEndoT) while knockdown of Oct4 by siRNA altering vascularization. In a rat MI model, overexpression of FoxC1 in ischemic hearts increased post-infarct vascular density and improved cardiac function. The transplantation of adOct4-pretreated MSCs into these ischemic niches augments MEndoT, enhanced vascularity, and further improved cardiac function. Consistently, these cardioprotective effects of FoxC1 was abrogated when Oct4 was depleted in the MSCs and was mimicked by overexpression of Oct4.

Conclusions: Together, these studies demonstrate that the FoxC1/Oct4 axis is an essential aspect for survival and neovascularization of MSCs in the ischemic conditions and represents a potential therapeutic target for enhancing cardiac repair.

Keywords: Angiogenesis; FoxC1; Hypoxic; Mesenchymal stem cells; Niche; Oct4.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Cells, Cultured
Endothelial Cells
Forkhead Transcription Factors
Mesenchymal Stem Cell Transplantation*
Mesenchymal Stem Cells*
Myocardial Ischemia* / genetics
Myocardial Ischemia* / therapy
Neovascularization, Physiologic
Octamer Transcription Factor-3 / genetics
Rats

Substances

Forkhead Transcription Factors
Foxc1 protein, rat
Octamer Transcription Factor-3
Pou5f1 protein, rat