Enhanced Cardioprotection by Human Endometrium Mesenchymal Stem Cells Driven by Exosomal MicroRNA-21

Kan Wang; Zhi Jiang; Keith A. Webster; Jinghai Chen; Hengxun Hu; Yu Zhou; Jing Zhao; Lihan Wang; Yingchao Wang; Zhiwei Zhong; Cheng Ni; Qingju Li; Charlie Xiang; Ling Zhang; Rongrong Wu; Wei Zhu; Hong Yu; Xinyang Hu; Jianan Wang

doi:10.5966/sctm.2015-0386

Enhanced Cardioprotection by Human Endometrium Mesenchymal Stem Cells Driven by Exosomal MicroRNA-21

Kan Wang(Zhejiang Lab), Zhi Jiang(Guizhou Provincial People's Hospital), Keith A. Webster(University of Miami), Jinghai Chen(Zhejiang Lab), Hengxun Hu(Zhejiang Lab), Yu Zhou(Zhejiang Lab), Jing Zhao(Zhejiang Lab), Lihan Wang(Zhejiang Lab), Yingchao Wang(Zhejiang Lab), Zhiwei Zhong(Zhejiang Lab), Cheng Ni(Zhejiang Lab), Qingju Li(Zhejiang Lab), Charlie Xiang(Zhejiang International Studies University), Ling Zhang(Zhejiang Lab), Rongrong Wu(Zhejiang Lab), Wei Zhu(Zhejiang Lab), Hong Yu(Zhejiang Lab), Xinyang Hu(Zhejiang Lab), Jianan Wang(Zhejiang Lab)

Stem Cells Translational Medicine

August 29, 2016

10.5966/sctm.2015-0386

Cited by 276Open Access

Full Text

Abstract

Our group recently reported positive therapeutic benefit of human endometrium-derived mesenchymal stem cells (EnMSCs) delivered to infarcted rat myocardium, an effect that correlated with enhanced secretion of protective cytokines and growth factors compared with parallel cultures of human bone marrow MSCs (BMMSCs). To define more precisely the molecular mechanisms of EnMSC therapy, in the present study, we assessed in parallel the paracrine and therapeutic properties of MSCs derived from endometrium, bone marrow, and adipose tissues in a rat model of myocardial infarction (MI). EnMSCs, BMMSCs, and adipose-derived MSCs (AdMSCs) were characterized by fluorescence-activated cell sorting (FACS). Paracrine and cytoprotective actions were assessed in vitro by coculture with neonatal cardiomyocytes and human umbilical vein endothelial cells. A rat MI model was used to compare cell therapy by intramyocardial injection of BMMSCs, AdMSCs, and EnMSCs. We found that EnMSCs conferred superior cardioprotection relative to BMMSCs or AdMSCs and supported enhanced microvessel density. Inhibitor studies indicated that the enhanced paracrine actions of EnMSCs were mediated by secreted exosomes. Analyses of exosomal microRNAs (miRs) by miR array and quantitative polymerase chain reaction revealed that miR-21 expression was selectively enhanced in exosomes derived from EnMSCs. Selective antagonism of miR-21 by anti-miR treatment abolished the antiapoptotic and angiogenic effects of EnMSCs with parallel effects on phosphatase and tensin homolog (PTEN), a miR-21 target and downstream Akt. The results of the present study confirm the superior cardioprotection by EnMSCs relative to BMMSCs or AdMSCs and implicates miR-21 as a potential mediator of EnMSC therapy by enhancing cell survival through the PTEN/Akt pathway. The endometrium might be a preferential source of MSCs for cardiovascular cell therapy. Stem Cells Translational Medicine 2017;6:209-222.

Related Papers

No related papers found

Powered by citation graph analysis