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Human Adipose-Derived Mesenchymal Stem Cells-Derived Exosomal microRNA-19b Promotes the Healing of Skin Wounds Through Modulation of the CCL1/TGF-β Signaling Axis

机译:人脂肪衍生的间充质干细胞衍生的外索体MicroRNA-19B通过调制CCL1 / TGF-β信号轴来促进皮肤伤口的愈合

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Introduction:Human adipose-derived mesenchymal stem cells (ADMSCs) with their secretory factors are able to induce collagen synthesis and fibroblast migration in the wound healing process. This study is launched to figure out the effect of human ADMSCs-derived exosomes on skin wound healing.Methods:ADMSCs were extracted and ADMSCs-derived exosomes were identified. Skin damage models were established by treating HaCaT cells and human skin fibroblasts with H 2 O 2 . Next, the roles of ADMSCs and their derived exosomes were investigated. The exosomal miRNA then was analyzed, and the function of miRNA on the H 2 O 2 -induced cells was studied by miRNA suppression. Bioinformatics analysis, luciferase activity and RIP assays were implemented to find the target genes ofthe miRNA and the modulated pathways. A mouse skin damage model was induced to elucidate the effects of exosomes in vivo by injecting exosomes.Results:H 2 O 2 treatment significantly reduced the viability of HaCaT cells and increased their apoptosis rate. Co-culture with ADMSCs or their derived exosomes could improve the cell damage caused by H 2 O 2 . Meanwhile, H 2 O 2 treatment promoted the internalization of exosomes. ADMSCs and their derived exosomes significantly increased miR-19b expression in the recipient cells, while inhibiting miR-19b resulted in a reduction in the therapeutic effect of ADMSCs-derived exosomes. Besides, miR-19b regulated the TGF-β pathway by targeting CCL1. The therapeutic effect of exosomes was further confirmed by a mouse model of skin damage.Conclusion:Our study indicates that exosomal miR-19b derived from ADMSCs regulates the TGF-β pathway by targeting CCL1, thereby promoting the healing of skin wounds.? 2020 Cao et al.
机译:介绍:人脂肪衍生的间充质干细胞(ADMSCs)具有其分泌因子能够在伤口愈合过程中诱导胶原合成和成纤维细胞迁移。推出该研究以弄清楚人类Admscs衍生的外来物体对皮肤伤口愈合的影响。方法:鉴定ADMSCS和ADMSCS衍生的外泌体。通过用H 2 O 2治疗HaCaT细胞和人体皮肤成纤维细胞来建立皮肤损伤模型。接下来,研究了ACMSCs及其衍生的外泌体的作用。然后分析外泌体miRNA,并通过miRNA抑制研究了MiRNA对H 2 O 2-2 O 2诱导细胞的功能。实施生物信息学分析,荧光素酶活性和RIP测定以找到miRNA和调制途径的靶基因。诱导小鼠皮肤损伤模型通过注射外来体内阐明外来体内的效果。结果:H 2 O 2治疗显着降低了HACAT细胞的活力并增加了它们的凋亡率。与ADMSCS或其衍生的外泌体的共同培养可以改善H 2 O 2引起的细胞损伤。同时,H 2 O 2治疗促进外来体的内化。 ADMSCS及其衍生的外来体显着增加了受体细胞中的miR-19b表达,同时抑制miR-19b导致ADMS衍生的外索体的治疗效果降低。此外,MIR-19B通过靶向CCL1调节TGF-β途径。进一步通过皮肤损伤的小鼠模型进一步证实外来的治疗效果。结论:我们的研究表明,通过靶向CCL1,衍生自ADSCs的外泌体miR-19b调节TGF-β途径,从而促进皮肤伤口的愈合。 2020 cao等。

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