Exosomal miR-223 Contributes to Mesenchymal Stem Cell-Elicited Cardioprotection in Polymicrobial Sepsis

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作者
Xiaohong Wang
Haitao Gu
Dongze Qin
Liwang Yang
Wei Huang
Kobina Essandoh
Yigang Wang
Charles C. Caldwell
Tianqing Peng
Basilia Zingarelli
Guo-Chang Fan
机构
[1] University of Cincinnati College of Medicine,Department of Pharmacology and Cell Biophysics
[2] University of Cincinnati College of Medicine,Department of Pathology and Laboratory Medicine
[3] University of Cincinnati College of Medicine,Department of Surgery
[4] Shanxi Medical University,Division of Critical Care Medicine
[5] Shanxi University of Traditional Chinese Medicine,undefined
[6] Critical Illness Research,undefined
[7] Lawson Health Research Institute,undefined
[8] Cincinnati Children’s Hospital Medical Center,undefined
来源
Scientific Reports | / 5卷
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摘要
Mesenchymal stem cells (MSCs) have been shown to elicit cardio-protective effects in sepsis. However, the underlying mechanism remains obscure. While recent studies have indicated that miR-223 is highly enriched in MSC-derived exosomes, whether exosomal miR-223 contributes to MSC-mediated cardio-protection in sepsis is unknown. In this study, loss-of-function approach was utilized and sepsis was induced by cecal ligation and puncture (CLP). We observed that injection of miR-223-KO MSCs at 1 h post-CLP did not confer protection against CLP-triggered cardiac dysfunction, apoptosis and inflammatory response. However, WT-MSCs were able to provide protection which was associated with exosome release. Next, treatment of CLP mice with exosomes released from miR-223-KO MSCs significantly exaggerated sepsis-induced injury. Conversely, WT-MSC-derived-exosomes displayed protective effects. Mechanistically, we identified that miR-223-KO exosomes contained higher levels of Sema3A and Stat3, two known targets of miR-223 (5p & 3p), than WT-exosomes. Accordingly, these exosomal proteins were transferred to cardiomyocytes, leading to increased inflammation and cell death. By contrast, WT-exosomes encased higher levels of miR-223, which could be delivered to cardiomyocytes, resulting in down-regulation of Sema3A and Stat3. These data for the first time indicate that exosomal miR-223 plays an essential role for MSC-induced cardio-protection in sepsis.
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