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氧饱和度和灌注变化在皮肤科氨甲酰基-L- 苏氨酸光动力治疗期间。

Oxygen saturation and perfusion changes during dermatological methylaminolaevulinate photodynamic therapy.

机构信息

Clinical Photobiology, European Centre for Environment and Human Health, Peninsula Medical School, University of Exeter, Royal Cornwall Hospital, Truro TR1 3HD, UK.

出版信息

Br J Dermatol. 2011 Dec;165(6):1323-31. doi: 10.1111/j.1365-2133.2011.10554.x. Epub 2011 Nov 17.

Abstract

BACKGROUND

Methylaminolaevulinate (MAL)-photodynamic therapy (PDT) is a successful topical treatment for a number of (pre)cancerous dermatological conditions. In combination, light of the appropriate wavelength, the photosensitizer protoporphyrin IX (PpIX) and tissue oxygen result in the production of singlet oxygen and reactive oxygen species inducing cell death.

OBJECTIVES

This study investigates real-time changes in localized tissue blood oxygen saturation and perfusion in conjunction with PpIX fluorescence monitoring for the first time during dermatological MAL-PDT.

METHODS

Oxygen saturation, perfusion and PpIX fluorescence were monitored noninvasively utilizing optical reflectance spectroscopy, laser Doppler perfusion imaging and a fluorescence imaging system, respectively. Patients attending for standard dermatological MAL-PDT were recruited to this ethically approved study and monitored prior to, during and after light irradiation.

RESULTS

Significant reductions in mean blood oxygen saturation (P < 0·005) and PpIX fluorescence (P < 0·001) were observed within the first minute of irradiation (4·75 J cm(-2) ) while, in contrast, perfusion was observed to increase significantly (P < 0·01) during treatment. The changes in oxygen saturation and PpIX fluorescence were positively correlated during the initial phase of treatment (r(2) = 0·766).

CONCLUSIONS

Rapid reductions in the localized blood oxygen saturation have been observed for the first time to occur clinically within the initial minutes of light irradiation and positively correlate with the concurrent PpIX photobleaching. Furthermore, perfusion increases, suggesting that the microvasculature compensates for the PDT-induced oxygen depletion.

摘要

背景

甲氨基酮戊酸(MAL)-光动力疗法(PDT)是治疗多种(癌前)皮肤病的成功局部治疗方法。在适当波长的光、光敏剂原卟啉 IX(PpIX)和组织氧的共同作用下,会产生单线态氧和活性氧,诱导细胞死亡。

目的

本研究首次在皮肤病 MAL-PDT 过程中,实时监测局部组织血氧饱和度和灌注的变化,并结合 PpIX 荧光监测。

方法

利用光学反射光谱、激光多普勒灌注成像和荧光成像系统分别对氧饱和度、灌注和 PpIX 荧光进行非侵入性监测。招募接受标准皮肤病 MAL-PDT 的患者,在照射前、照射中和照射后进行监测。

结果

在第一次照射(4.75 J cm(-2))的最初一分钟内,观察到平均血氧饱和度(P < 0.005)和 PpIX 荧光(P < 0.001)显著降低,而在治疗过程中,灌注则显著增加(P < 0.01)。在治疗的初始阶段,氧饱和度和 PpIX 荧光的变化呈正相关(r(2) = 0.766)。

结论

首次观察到,在初始光照射的最初几分钟内,局部血氧饱和度迅速降低,与同时发生的 PpIX 光漂白呈正相关。此外,灌注增加,表明微血管系统补偿了 PDT 引起的氧耗竭。

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