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首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >Lucidone Promotes the Cutaneous Wound Healing Process via Activation of the PI3K/AKT, Wnt/beta-catenin and NF-kappa B Signaling Pathways
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Lucidone Promotes the Cutaneous Wound Healing Process via Activation of the PI3K/AKT, Wnt/beta-catenin and NF-kappa B Signaling Pathways

机译:Lucidone 通过激活 PI3K/AKT、Wnt/β-catenin 和 NF-κ B 信号通路促进皮肤伤口愈合过程

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Lucidone, which comprises a naturally occurring cyclopentenedione, has been investigated for its in vitro and in vivo wound healing properties, and the underlying molecular signaling cascades in the wound healing mechanism have been elucidated. We demonstrated the cell-/dose-specific responses of lucidone (0.5-8 mu M) on proliferation and migration/invasion of keratinocyte HaCaT and fibroblast Hs68 cells. In keratinocytes, lucidone-induced nuclear translocation of beta-catenin was accompanied by increased transcriptional target genes, including c-Myc and cyclin-D1, through GSK3 beta-dependent pathway. Correspondingly, lucidone promoted the cell-cycle by increasing PCNA/CDK4 and decreasing p21/p27 expressions. Lucidone induced EMT through the downregulation of epithelial (E-cadherin/occludin) and upregulation of mesenchymal (vimentin/Twist/Snail) marker proteins. Activated MMP-9/-2 and uPA/uPAR as well as suppressed TIMP-1/-2 and PAI-1 expressions by lucidone may promote the migration/invasion of keratinocytes. Notably, lucidone activated NF-kappa B signaling via IKK-mediated-I kappa B degradation, and its inhibition abolished MMP-9 activation and keratinocyte migration. Inhibition of PI3K/AKT signaling impaired the lucidone-induced proliferation/migration with corresponding suppression of beta-catenin/c-Myc/cyclin-D1 and NF-kappa B/MMP-9 expressions. Results indicate that lucidone-induced PI3K/AKT signaling anchored the beta-catenin/NF-kappa B-mediated healing mechanism. beta-catenin knockdown substantially diminished lucidone-induced keratinocyte migration. Furthermore, lucidone increased endothelial cell proliferation/migration and triggered angiogenesis (MMP-9/uPA/ICAM-1). In macrophages, lucidone-activated NF-kappa B-mediated inflammation (COX-2/iNOS/NO) and VEGF, which may contribute to the growth of keratinocytes/fibroblasts and endothelial cells. Punched wounds on mice were rapidly healed with the topical application of lucidone (5 mM) compared with control ointment-treated mice. Taken together, lucidone accelerates wound healing through the cooperation of keratinocyte/fibroblast/endothelial cell growth and migration and macrophage inflammation via PI3K/AKT, Wnt/beta-catenin and NF-kappa B signaling cascade activation. (C) 2016 Elsevier B.V. All rights reserved.
机译:Lucidone由天然存在的环戊二酮组成,已经研究了其体外和体内伤口愈合特性,并阐明了伤口愈合机制中潜在的分子信号级联。我们证明了荧光酮 (0.5-8 μ M) 对角质形成细胞 HaCaT 和成纤维细胞 Hs68 细胞增殖和迁移/侵袭的细胞/剂量特异性反应。在角质形成细胞中,荧光素诱导的β-连环蛋白核易位伴随着转录靶基因的增加,包括c-Myc和cyclin-D1,通过GSK3β依赖性途径。相应地,清醒酮通过增加PCNA/CDK4和降低p21/p27表达来促进细胞周期。Lucidone 通过下调上皮 (E-cadherin/occludin) 和上调间充质 (vimentin/Twist/Snail) 标记蛋白来诱导 EMT。激活的 MMP-9/-2 和 uPA/uPAR 以及清醒酮抑制的 TIMP-1/-2 和 PAI-1 表达可能促进角质形成细胞的迁移/侵袭。值得注意的是,芈酮通过 IKK 介导的 I κ B 降解激活 NF-κ B 信号传导,其抑制消除了 MMP-9 激活和角质形成细胞迁移。抑制 PI3K/AKT 信号转导损害了荧光素诱导的增殖/迁移,并相应抑制了 β-连环蛋白/c-Myc/细胞周期蛋白-D1 和 NF-κ B/MMP-9 的表达。结果表明,荧光素诱导的PI3K/AKT信号转导锚定了β-连环蛋白/NF-κB介导的愈合机制。β-连环蛋白敲低显著减少了荧光素诱导的角质形成细胞迁移。此外,芉酮增加内皮细胞增殖/迁移并触发血管生成 (MMP-9/uPA/ICAM-1)。在巨噬细胞中,荧光素激活的NF-κ B介导的炎症(COX-2/iNOS/NO)和VEGF,可能有助于角质形成细胞/成纤维细胞和内皮细胞的生长。与对照软膏治疗的小鼠相比,局部应用lucidone(5mM)可快速愈合小鼠的打孔伤口。综上所述,芈酮通过角质形成细胞/成纤维细胞/内皮细胞生长和迁移以及巨噬细胞炎症的合作,通过PI3K/AKT、Wnt/β-catenin和NF-κ B信号级联激活来加速伤口愈合。(C) 2016 Elsevier B.V.保留所有权利。

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