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比较肢端和非肢端部位皮肤肿瘤在甲氨基酮戊酸光动力疗法中卟啉IX 的积累和破坏。

Comparison of protoporphyrin IX accumulation and destruction during methylaminolevulinate photodynamic therapy of skin tumours located at acral and nonacral sites.

机构信息

Clinical Photobiology, European Centre of Environment and Human Health, Peninsula Medical School, University of Exeter, Royal Cornwall Hospital, Treliske, Truro, Cornwall, UK.

出版信息

Br J Dermatol. 2011 Jun;164(6):1362-8. doi: 10.1111/j.1365-2133.2011.10265.x. Epub 2011 May 13.

Abstract

BACKGROUND

Topical photodynamic therapy (PDT) is successful in the treatment of nonmelanoma skin cancers and associated precancers, but efficacy is significantly reduced in actinic keratosis lesions not located on the face or scalp.

OBJECTIVES

To compare the changes in protoporphyrin IX (PpIX) fluorescence in lesions undergoing routine methylaminolevulinate (MAL) PDT and the clinical outcome observed 3 months after treatment in lesions located at acral and nonacral sites.

METHODS

This study was a noninterventional, nonrandomized, observational study, which monitored changes in PpIX fluorescence in 200 lesions during standard dermatological MAL-PDT. These data were subsequently analysed in terms of lesions located at acral and nonacral sites.

RESULTS

Clinical clearance was significantly reduced (P < 0·01) in acral skin lesions when compared with lesions located at nonacral sites. The accumulation and destruction of PpIX fluorescence was significantly reduced in these acral lesions (P < 0·05 and P < 0·001, respectively). Specifically, lesion location at acral sites significantly reduced changes in PpIX fluorescence in actinic keratosis lesions during MAL-PDT (P < 0·01 and P < 0·05).

CONCLUSIONS

These data suggest that reduced PpIX accumulation and the subsequent reduction in PpIX photobleaching within acral lesions result in the reduced responsiveness of these lesions to MAL-PDT. Future work should therefore aim to improve photosensitizer accumulation/photobleaching within lesions located at acral sites.

摘要

背景

局部光动力疗法(PDT)在治疗非黑素瘤皮肤癌及其相关癌前病变方面取得了成功,但在非面部或头皮的光化性角化病病变中,疗效显著降低。

目的

比较常规氨甲酰基-L-丙氨酸(MAL)PDT 治疗过程中病变中原卟啉 IX(PpIX)荧光的变化,以及治疗 3 个月后非肢端和肢端部位病变的临床结果。

方法

这是一项非干预性、非随机、观察性研究,监测了 200 个病变在标准皮肤科 MAL-PDT 过程中 PpIX 荧光的变化。随后根据病变位于肢端和非肢端部位对这些数据进行了分析。

结果

与非肢端部位的病变相比,肢端皮肤病变的临床清除率显著降低(P < 0·01)。这些肢端病变中 PpIX 荧光的积累和破坏明显减少(P < 0·05 和 P < 0·001)。具体来说,病变位于肢端部位显著降低了 MAL-PDT 中光化性角化病病变中 PpIX 荧光的变化(P < 0·01 和 P < 0·05)。

结论

这些数据表明,肢端病变中 PpIX 积累减少以及随后的 PpIX 光漂白减少导致这些病变对 MAL-PDT 的反应性降低。因此,未来的工作应旨在改善位于肢端部位的病变中光敏剂的积累/光漂白。

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