首页> 美国卫生研究院文献>Redox Biology >MnSOD is implicated in accelerated wound healing upon Negative Pressure Wound Therapy (NPWT): A case in point for MnSOD mimetics as adjuvants for wound management
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MnSOD is implicated in accelerated wound healing upon Negative Pressure Wound Therapy (NPWT): A case in point for MnSOD mimetics as adjuvants for wound management

机译:MnSOD涉及负压伤口治疗(NPWT)的加速伤口愈合:以MnSOD模拟物作为伤口处理佐剂的一个例子

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摘要

Negative Pressure Wound Therapy (NPWT), a widely used modality in the management of surgical and trauma wounds, offers clear benefits over conventional wound healing strategies. Despite the wide-ranging effects ascribed to NPWT, the precise molecular mechanisms underlying the accelerated healing supported by NPWT remains poorly understood. Notably, cellular redox status-a product of the balance between cellular reactive oxygen species (ROS) production and anti-oxidant defense systems-plays an important role in wound healing and dysregulation of redox homeostasis has a profound effect on wound healing. Here we investigated potential links between the use of NPWT and the regulation of antioxidant mechanisms. Using patient samples and a rodent model of acute injury, we observed a significant accumulation of MnSOD protein as well as higher enzymatic activity in tissues upon NPWT. As a proof of concept and to outline the important role of SOD activity in wound healing, we replaced NPWT by the topical application of a MnSOD mimetic, Mn(III) meso-tetrakis(N-ethylpyridinium-2-yl)porphyrin (MnTE-2-PyP5+, MnE, BMX-010, AEOl10113) in the rodent model. We observed that MnE is a potent wound healing enhancer as it appears to facilitate the formation of new tissue within the wound bed and consequently advances wound closure by two days, compared to the non-treated animals. Taken together, these results show for the first time a link between NPWT and regulation of antioxidant mechanism through the maintenance of MnSOD activity. Additionally this discovery outlined the potential role of MnSOD mimetics as topical agents enhancing wound healing.
机译:负压伤口治疗(NPWT)是一种在外科手术和创伤伤口处理中广泛使用的方式,与传统的伤口愈合策略相比,具有明显的优势。尽管NPWT产生了广泛的影响,但NPWT支持的加速愈合的确切分子机制仍知之甚少。值得注意的是,细胞氧化还原状态-细胞活性氧(ROS)产生与抗氧化防御系统之间的平衡产物-在伤口愈合中起重要作用,氧化还原稳态的失调对伤口愈合有深远的影响。在这里,我们调查了NPWT的使用与抗氧化剂机制的调节之间的潜在联系。使用患者样品和啮齿动物急性损伤模型,我们观察到NPWT后MnSOD蛋白大量积累,并且组织中的酶活性更高。作为概念的证明并概述SOD活性在伤口愈合中的重要作用,我们通过局部应用MnSOD模拟物Mn(III)中四(N-乙基吡啶-2-基)卟啉(MnTE-啮齿动物模型中的2-PyP 5 + ,MnE,BMX-010,AEO11013)。我们观察到,MnE是一种有效的伤口愈合促进剂,因为与未治疗的动物相比,MnE似乎促进了伤口床内新组织的形成,从而使伤口闭合提前了两天。总而言之,这些结果首次显示了NPWT与通过维持MnSOD活性来调节抗氧化机制之间的联系。此外,该发现概述了MnSOD模拟物作为促进伤口愈合的局部用药的潜在作用。

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