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Cold Atmospheric Plasma (CAP) Changes Gene Expression of Key Molecules of the Wound Healing Machinery and Improves Wound Healing In Vitro and In Vivo

机译:冷大气血浆(CAP)改变伤口愈合机械关键分子的基因表达并改善体内和体外伤口愈合

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摘要

Cold atmospheric plasma (CAP) has the potential to interact with tissue or cells leading to fast, painless and efficient disinfection and furthermore has positive effects on wound healing and tissue regeneration. For clinical implementation it is necessary to examine how CAP improves wound healing and which molecular changes occur after the CAP treatment. In the present study we used the second generation MicroPlaSter ß® in analogy to the current clinical standard (2 min treatment time) in order to determine molecular changes induced by CAP using in vitro cell culture studies with human fibroblasts and an in vivo mouse skin wound healing model. Our in vitro analysis revealed that the CAP treatment induces the expression of important key genes crucial for the wound healing response like IL-6, IL-8, MCP-1, TGF-ß1, TGF-ß2, and promotes the production of collagen type I and alpha-SMA. Scratch wound healing assays showed improved cell migration, whereas cell proliferation analyzed by XTT method, and the apoptotic machinery analyzed by protein array technology, was not altered by CAP in dermal fibroblasts. An in vivo wound healing model confirmed that the CAP treatment affects above mentioned genes involved in wound healing, tissue injury and repair. Additionally, we observed that the CAP treatment improves wound healing in mice, no relevant side effects were detected. We suggest that improved wound healing might be due to the activation of a specified panel of cytokines and growth factors by CAP. In summary, our in vitro human and in vivo animal data suggest that the 2 min treatment with the MicroPlaSter ß® is an effective technique for activating wound healing relevant molecules in dermal fibroblasts leading to improved wound healing, whereas the mechanisms which contribute to these observed effects have to be further investigated.
机译:寒冷的大气血浆(CAP)可能与组织或细胞相互作用,从而导致快速,无痛且有效的消毒,并且还对伤口愈合和组织再生产生积极影响。对于临床实施,有必要检查CAP如何改善伤口愈合以及CAP治疗后会发生哪些分子变化。在本研究中,我们以类似于当前临床标准的标准(2分钟的治疗时间)使用了第二代MicroPlaSterß®,以确定使用人成纤维细胞和体内小鼠皮肤伤口进行的体外细胞培养研究,确定由CAP诱导的分子变化。修复模型。我们的体外分析显示,CAP处理可诱导对伤口愈合反应至关重要的重要关键基因的表达,例如IL-6,IL-8,MCP-1,TGF-ß1,TGF-ß2,并促进胶原类型的产生我和alpha-SMA。从头开始的伤口愈合试验显示出改善的细胞迁移,而通过XTT方法分析的细胞增殖以及通过蛋白质阵列技术分析的凋亡机制并未受到CAP在真皮成纤维细胞中的改变。体内伤口愈合模型证实,CAP治疗影响上述涉及伤口愈合,组织损伤和修复的基因。此外,我们观察到CAP治疗可改善小鼠的伤口愈合,未检测到相关的副作用。我们建议改善伤口愈合可能是由于CAP激活了特定的一组细胞因子和生长因子。总而言之,我们的体外人和体内动物数据表明,用MicroPlaSterß®处理2分钟是激活皮肤成纤维细胞中伤口愈合相关分子的有效技术,从而改善了伤口愈合,而观察到这些现象的机制效果有待进一步调查。

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