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Development of a handheld fluorescence imaging device to investigate the characteristics of protoporphyrin IX fluorescence in healthy and diseased skin

机译:开发用于研究健康和患病皮肤中原卟啉IX荧光特性的手持式荧光成像设备

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摘要

BackgroundTopical Photodynamic therapy (PDT) is an effective treatment for superficial non-melanoma skin cancers (NMSC) and dysplasia. During PDT light activates the photosensitiser (PpIX), metabolised from a topical pro-drug. A combination of PpIX, light and molecular oxygen results in inflammation and cell death. However, the outcomes of the treatment could be better. Insufficient biosynthesis of PpIX may be one of the causes of incomplete response or recurrence. Measuring surface fluorescence is usually employed as a means of studying PpIX formation. The aim of this work was to develop a device and a method for convenient fluorescence imaging in clinical settings to gather information on PpIX metabolism in healthy skin and NMSC with a view to improving PDT regimes.MethodsA handheld fluorescence camera and a time course imaging method was developed and used in healthy volunteers and patients diagnosed with basal cell carcinoma (BCC) and actinic keratosis (AK). The photosensitiser (precursor) creams used were 5-aminolaevulinic acid (ALA; Ameluz®) and methyl aminolevulinate (MAL; Metvix®). Pain was assessed using a visual analogue score immediately after the PDT.ResultsFluorescence due to PpIX increases over three hours incubation in healthy skin and in lesional BCC and AK. Distribution of PpIX fluorescence varies between the lesion types and between subjects. There was no significant correlation between PpIX fluorescence characteristics and pro-drug, diagnosis or pain experienced. However, there was a clear dependence on body site.ConclusionThe device and the method developed can be used to assess the characteristics of PpIX fluorescence, quantitative analysis and time course. Our findings show that body site influences PpIX fluorescence which we suggest may be due to the difference in skin temperature at different body sites.
机译:背景技术局部光动力疗法(PDT)是治疗浅表非黑色素瘤皮肤癌(NMSC)和发育异常的有效疗法。在PDT期间,光会激活从局部前药代谢的光敏剂(PpIX)。 PpIX,光和分子氧的组合会导致炎症和细胞死亡。但是,治疗结果可能会更好。 PpIX的生物合成不足可能是不完全应答或复发的原因之一。测量表面荧光通常被用作研究PpIX形成的一种手段。这项工作的目的是开发一种在临床环境中方便地进行荧光成像的设备和方法,以收集有关健康皮肤和NMSC中PpIX代谢的信息,从而改善PDT的状况。开发并用于健康志愿者和诊断为基底细胞癌(BCC)和光化性角化病(AK)的患者。使用的光敏剂(前体)乳霜是5-氨基戊酸(ALA;Ameluz®)和氨基乙酰丙酸甲酯(MAL;)。在PDT后立即使用视觉模拟评分评估疼痛。结果在健康皮肤以及病变的BCC和AK中孵育3小时后,由于PpIX引起的荧光增加。 PpIX荧光的分布在病变类型之间和受试者之间有所不同。 PpIX荧光特征与前药,诊断或经历的疼痛之间无显着相关性。结论所开发的装置和方法可用于评估PpIX荧光的特征,定量分析和时间过程。我们的发现表明,身体部位会影响PpIX荧光,我们认为这可能是由于不同身体部位的皮肤温度不同所致。

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