间接暴露非热等离子体装置的化学剂量测定

S. Plimpton, M. Gołkowski, Chad M. Austin, M. Voskuil, Deborah G. Mitchell, S. Eaton, G. Eaton, C. Golkowski
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引用次数: 0

摘要

只提供摘要形式。对在生物医学环境中使用非热等离子体的兴趣正在迅速增长。这种装置的潜在应用范围从器械灭菌到临床治疗。实施非热等离子体的最大障碍之一,特别是在患者接触方面,是对发生的化学过程的理解相对较差。最近的研究集中在与特定放电结构相关的动态化学混合物上。我们的团队最近详细介绍了通过修改操作参数(即湿度)来控制我们的设备产生的化学物质的能力。具体来说,我们展示了我们的设备能够将短寿命的羟基自由基输送到距离等离子体放电超过一米的治疗点。我们的远程设计的最新发展允许潜在的用户自定义特异性的浓度和风味的化学暴露于处理环境。将非热等离子体装置引入临床环境,特别是在美国,将不可避免地需要一定程度的治疗控制。我们报道了与我们的设备应用相关的体外“血浆剂量学”。控制装置流出物的化学组成允许参数化处理相关变量,如原核生物和真核生物物种之间的失活或DNA氧化比率。在先前的工作基础上,利用电子自旋共振光谱来枚举传递到我们治疗部位的自由基,我们展示了治疗操作窗口的潜力。这种调节提供了针对正在治疗的污染或感染调整基于非热等离子体的设备的潜力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Chemical dosimetry of an indirect exposure non-thermal plasma device
Summary form only given. Interest in the use of non-thermal plasmas in the biomedical setting is rapidly growing. Potential applications of such devices range from instrument sterilization to clinical therapy. One of the largest hurdles to the implementation of nonthermal plasmas, specifically in regard to patient exposure, is the relatively poor understanding of the chemical processes taking place. Recent research has focused intensely on the dynamic chemical cocktail associated with specific discharge configurations. Our group recently detailed the ability to control chemical species created by our device through modifying operating parameters, namely humidity1. Specifically, we demonstrated our device's capability to deliver the short-lived hydroxyl radical to treatment sites at a distance of over a meter from the plasma discharge. This recent development of our remote design allows for potential user-defined specificity in both concentration and flavor of chemical exposure to the treatment environment. Introduction of non-thermal plasma devices to the clinical setting, specifically in the United States, will inevitably require a certain degree of therapeutic control. We report on the in vitro “plasma dosimetry” related to the application of our device. Control of the device effluent's chemical makeup allows for parameterization of treatment-related variables like the ratio of inactivation or DNA oxidation between prokaryotic and eukaryotic species. Building on previous work using electron spin resonance spectroscopy to enumerate free radicals delivered to our treatment site, we demonstrate the potential for a therapeutic window of operation. Such regulation provides the potential to tune non-thermal plasma based devices with regard to the contamination or infection being treated.
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