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光动力疗法期间氧监测的作用及其在治疗剂量测定中的潜力。

The role of oxygen monitoring during photodynamic therapy and its potential for treatment dosimetry.

作者信息

Woodhams Josephine H, Macrobert Alexander J, Bown Stephen G

机构信息

National Medical Laser Centre, Royal Free and University College Medical School, University College London, Charles Bell House, 67-73 Riding House Street, London, UKW1W 7EJ.

出版信息

Photochem Photobiol Sci. 2007 Dec;6(12):1246-56. doi: 10.1039/b709644e. Epub 2007 Sep 21.

Abstract

Understanding of the biology of photodynamic therapy (PDT) has expanded tremendously over the past few years. However, in the clinical situation, it is still a challenge to match the extent of PDT effects to the extent of the disease process being treated. PDT requires drug, light and oxygen, any of which can be the limiting factor in determining efficacy at each point in a target organ. This article reviews techniques available for monitoring tissue oxygenation during PDT. Point measurements can be made using oxygen electrodes or luminescence-based optodes for direct measurements of tissue pO2, or using optical spectroscopy for measuring the oxygen saturation of haemoglobin. Imaging is considerably more complex, but may become feasible with techniques like BOLD MRI. Pre-clinical studies have shown dramatic changes in oxygenation during PDT, which vary with the photosensitizer used and the light delivery regimen. Better oxygenation throughout treatment is achieved if the light fluence rate is kept low as this reduces the rate of oxygen consumption. The relationship between tissue oxygenation and PDT effect is complex and remarkably few studies have directly correlated oxygenation changes during PDT with the final biological effect, although those that have confirm the value of maintaining good oxygenation. Real time monitoring to ensure adequate oxygenation at strategic points in target tissues during PDT is likely to be important, particularly in the image guided treatment of tumours of solid organs.

摘要

在过去几年中,人们对光动力疗法(PDT)生物学的理解有了极大的拓展。然而,在临床实际中,要使PDT的治疗效果与所治疗疾病进程的程度相匹配,仍然是一项挑战。PDT需要药物、光和氧气,其中任何一种都可能成为决定靶器官中每个点疗效的限制因素。本文综述了PDT过程中监测组织氧合的可用技术。点测量可使用氧电极或基于发光的光极直接测量组织的氧分压(pO2),或使用光谱学测量血红蛋白的氧饱和度。成像要复杂得多,但像血氧水平依赖性功能磁共振成像(BOLD MRI)这样的技术可能使其变得可行。临床前研究表明,PDT过程中氧合会发生显著变化,这些变化因所用光敏剂和光传递方案而异。如果光通量率保持较低,整个治疗过程中会实现更好的氧合,因为这会降低氧消耗率。组织氧合与PDT效果之间的关系很复杂,尽管那些证实维持良好氧合价值的研究表明,直接将PDT过程中的氧合变化与最终生物学效应相关联的研究非常少。在PDT期间对靶组织中的关键部位进行实时监测以确保充足的氧合可能很重要,尤其是在实体器官肿瘤的图像引导治疗中。

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