EGCG ameliorates the hypoxia-induced apoptosis and osteogenic differentiation reduction of mesenchymal stem cells via upregulating miR-210
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  • 作者:Yiyan Qiu ; Yang Chen ; Tenghui Zeng ; Weizhuang Guo ; Wenyu Zhou…
  • 关键词:EGCG ; miR ; 210 ; Apoptosis ; Osteogenic differentiation ; Mesenchymal stem cells ; EFNA3
  • 刊名:Molecular Biology Reports
  • 出版年:2016
  • 出版时间:March 2016
  • 年:2016
  • 卷:43
  • 期:3
  • 页码:183-193
  • 全文大小:1,395 KB
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  • 作者单位:Yiyan Qiu (1)
    Yang Chen (1)
    Tenghui Zeng (1)
    Weizhuang Guo (1)
    Wenyu Zhou (1)
    Xinjian Yang (1)

    1. Department of Spine Surgery, The 2nd Shenzhen People’s Hospital, No. 3002, Sungang Road, Futian District, Shenzhen, 510000, China
  • 刊物类别:Biomedical and Life Sciences
  • 刊物主题:Life Sciences
    Animal Anatomy, Morphology and Histology
    Animal Biochemistry
  • 出版者:Springer Netherlands
  • ISSN:1573-4978
文摘
The healing process of fractured bone is affected by the multiple factors regulating the growth and differentiation of osteoblasts and bone mesenchymal stem cells (MSCs), however, such markers and molecular events need to be orchestrated in details. This study investigated the effect of polyphenol(-)-epigallocatechin-3-gallate (EGCG) on the hypoxia-induced apoptosis and osteogenic differentiation of human bone marrow-derived MSCs, examined the miR-210 induction by EGCG, explored the target inhibition of the expression of receptor tyrosine kinase ligand ephrin-A3 (EFNA3) by miR-210, and then determined the association of the miR-210 promotion with the hypoxia-induced apoptosis and osteogenic differentiation. Results demonstrated that EGCG treatment significantly inhibited the hypoxia-induced apoptosis in MSCs and promoted the level of alkaline phosphatase (ALP), bone morphogenetic protein 2 (BMP-2), propeptide of type I procollagen I (PINP) and runt-related transcription factor 2 (RUNX2) in MSCs under either normoxia or hypoxia. Moreover, the EGCG treatment upregulated the miR-210 expression, in an association with EFNA3 downregulation; and the miR-210 upregulation significantly downregulated the expression of EFNA3 via the specific binding to the 3′ UTR of EFNA3. In addition, the manipulated miR-210 upregulation exerted amelioration on the hypoxia-induced apoptosis and on the hypoxia-reduced expression of ALP, BMP-2, PINP and RUNX2 in MSCs. In summary, our study indicated the protective role of EGCG in response to hypoxia and promontory role to osteogenic differentiation in MSCs via upregulating miR-210 and downregulating the expression of miR-210-targeted EFNA3. Our study implies the protective role of EGCG in the hypoxia-induced impairment in MSCs.

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