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Angiogenesis Is Induced and Wound Size Is Reduced by Electrical Stimulation in an Acute Wound Healing Model in Human Skin

机译:在人类皮肤急性伤口愈合模型中通过电刺激诱导血管生成并减小伤口尺寸

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摘要

Angiogenesis is critical for wound healing. Insufficient angiogenesis can result in impaired wound healing and chronic wound formation. Electrical stimulation (ES) has been shown to enhance angiogenesis. We previously showed that ES enhanced angiogenesis in acute wounds at one time point (day 14). The aim of this study was to further evaluate the role of ES in affecting angiogenesis during the acute phase of cutaneous wound healing over multiple time points. We compared the angiogenic response to wounding in 40 healthy volunteers (divided into two groups and randomised), treated with ES (post-ES) and compared them to secondary intention wound healing (control). Biopsy time points monitored were days 0, 3, 7, 10, 14. Objective non-invasive measures and H&E analysis were performed in addition to immunohistochemistry (IHC) and Western blotting (WB). Wound volume was significantly reduced on D7, 10 and 14 post-ES (p = 0.003, p = 0.002, p<0.001 respectively), surface area was reduced on days 10 (p = 0.001) and 14 (p<0.001) and wound diameter reduced on days 10 (p = 0.009) and 14 (p = 0.002). Blood flow increased significantly post-ES on D10 (p = 0.002) and 14 (p = 0.001). Angiogenic markers were up-regulated following ES application; protein analysis by IHC showed an increase (p<0.05) in VEGF-A expression by ES treatment on days 7, 10 and 14 (39%, 27% and 35% respectively) and PLGF expression on days 3 and 7 (40% on both days), compared to normal healing. Similarly, WB demonstrated an increase (p<0.05) in PLGF on days 7 and 14 (51% and 35% respectively). WB studies showed a significant increase of 30% (p>0.05) on day 14 in VEGF-A expression post-ES compared to controls. Furthermore, organisation of granulation tissue was improved on day 14 post-ES. This randomised controlled trial has shown that ES enhanced wound healing by reduced wound dimensions and increased VEGF-A and PLGF expression in acute cutaneous wounds, which further substantiates the role of ES in up-regulating angiogenesis as observed over multiple time points. This therapeutic approach may have potential application for clinical management of delayed and chronic wounds.
机译:血管生成对于伤口愈合至关重要。血管生成不足会导致伤口愈合不良和慢性伤口形成。电刺激(ES)已显示增强血管生成。我们先前显示,ES可在某一时间点(第14天)增强急性伤口的血管生成。这项研究的目的是进一步评估ES在多个时间点皮肤伤口愈合的急性期中影响血管生成的作用。我们比较了40名健康志愿者(分为两组并随机分组),ES治疗(ES后)对创面的血管生成反应,并将其与次要目的伤口愈合(对照)进行比较。监测的活检时间点是第0、3、7、10、14天。除了免疫组织化学(IHC)和蛋白质印迹(WB)之外,还进行了客观的非侵入性测量和H&E分析。 ES后第7天,第10天和第14天伤口体积显着减少(分别为p = 0.003,p = 0.002,p <0.001),在第10天(p = 0.001)和第14天表面积减小(p <0.001),并伤口第10天(p = 0.009)和第14天(p = 0.002)直径减小。 ES后D10(p = 0.002)和14(p = 0.001)时血流量显着增加。 ES应用后,血管生成标志物被上调。通过IHC进行的蛋白分析显示,ES处理后第7、10和14天(分别为39%,27%和35%)和PLGF表达在第3天和第7天(分别为40%和40%)增加(p <0.05)两天),相比于正常愈合。同样,WB在第7天和第14天显示PLGF增加(p <0.05)(分别为51%和35%)。 WB研究显示,与对照组相比,ES后VEGF-A表达在第14天显着增加了30%(p> 0.05)。此外,ES后第14天肉芽组织的组织得到改善。这项随机对照试验表明,ES通过减少伤口尺寸和增加急性皮肤伤口中的VEGF-A和PLGF表达来增强伤口愈合,进一步证实了ES在多个时间点上调血管新生的作用。这种治疗方法可能在延迟和慢性伤口的临床管理中具有潜在的应用。

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