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一种用于黑素瘤光动力治疗的新方法——紫光光动力治疗的色素脱失效果

A new method for photodynamic therapy of melanotic melanoma -- effects of depigmentation with violet light photodynamic therapy.

作者信息

Ma Li-Wei, Nielsen Kristian Pagh, Iani Vladimir, Moan Johan

机构信息

Department of Radiation Biophysics, Institute for Cancer Research, Rikshospital-Radiumhospital HF and Plasma/Room Physics, University of Oslo, Oslo, Norway.

出版信息

J Environ Pathol Toxicol Oncol. 2007;26(3):165-72. doi: 10.1615/jenvironpatholtoxicoloncol.v26.i3.10.

Abstract

Melanotic melanomas have a poor response to photodynamic therapy (PDT). The reason for this is that melanin absorbs light over the entire wavelength region used for PDT (400-750 nm). Photobleaching of melanin is an approach to overcome this obstacle. In the present work, reflectance spectroscopy was applied to study depigmentation of human and murine skin with different melanin contents, and effects induced by PDT with topical application of methyl 5-aminolevulinate (MAL) on B16F10 melanotic melanomas transplanted to nude mice. Depigmentation and inhibition of tumor growth after violet light (420 nm) exposure, red light (634 nm) exposure, and combinations of both were studied. Reflectance spectroscopy was suitable for evaluation of the pigmentation of both human and murine skin. Skin depigmentation leads to increase in reflectance. PDT with violet light bleached some of the melanin in the skin above the B16F10 melanomas, and possibly also in the upper part of the melanomas. This resulted in a larger growth inhibition of tumors first given PDT with violet light and then with red light compared to treatments using the reverse order of illumination, namely, red light before violet light. It is concluded that violet light PDT can bleach melanin in melanotic tumors and therefore increase their sensitivity to red light PDT. This finding indicates a new PDT modality that can be further developed for treatment of superficial melanotic melanomas and possibly other diseases where pigmentation is a problem.

摘要

黑素性黑色素瘤对光动力疗法(PDT)反应不佳。其原因在于黑色素在用于PDT的整个波长区域(400 - 750纳米)都能吸收光。黑色素的光漂白是克服这一障碍的一种方法。在本研究中,应用反射光谱法研究了不同黑色素含量的人和小鼠皮肤的色素脱失情况,以及局部应用5 - 氨基乙酰丙酸甲酯(MAL)进行PDT对移植到裸鼠身上的B16F10黑素性黑色素瘤的影响。研究了紫光(420纳米)照射、红光(634纳米)照射以及两者联合照射后色素脱失和肿瘤生长抑制情况。反射光谱法适用于评估人和小鼠皮肤的色素沉着。皮肤色素脱失会导致反射率增加。用紫光进行的PDT使B16F10黑色素瘤上方皮肤中的一些黑色素发生了光漂白,可能也使黑色素瘤上部的黑色素发生了光漂白。与采用相反照射顺序(即先红光后紫光)的治疗相比,先进行紫光PDT然后进行红光PDT的治疗对肿瘤生长的抑制作用更大。得出的结论是,紫光PDT可使黑素性肿瘤中的黑色素发生光漂白,从而提高其对红光PDT的敏感性。这一发现表明了一种新的PDT模式,可进一步开发用于治疗浅表黑素性黑色素瘤以及可能存在色素沉着问题的其他疾病。

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