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Noninvasive Optical Imaging of UV-Induced Squamous Cell Carcinoma in Murine Skin: Studies of Early Tumor Development and Vitamin D Enhancement of Protoporphyrin IX Production

机译:紫外线诱导的小鼠皮肤鳞状细胞癌的无创光学成像:肿瘤早期发展和维生素D增强原卟啉IX产生的研究

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摘要

Better noninvasive techniques are needed to monitor protoporphyrin IX (PpIX) levels before and during photodynamic therapy (PDT) of squamous cell carcinoma (SCC) of the skin. Our aim was to evaluate: (1) multispectral fluorescent imaging of ultraviolet light (UV)-induced cancer and precancer in a mouse model of SCC; (2) multispectral imaging and probe-based fluorescence detection as a tool to study Vitamin D (VD) effects on aminolevulinic acid (ALA)-induced PpIX synthesis. Dorsal skin of hairless mice was imaged weekly during a 24-week UV carcinogenesis protocol. Hot spots of PpIX fluorescence were detectable by multispectral imaging beginning at 14 weeks of UV exposure. Many hot spots disappeared after cessation of UV at week 20, but others persisted or became visible after week 20, and corresponded to tumors that eventually became visible by eye. In SCC-bearing mice pretreated with topical VD before ALA application, our optical techniques confirmed that VD preconditioning induces a tumor-selective increase in PpIX levels. Fluorescence-based optical imaging of PpIX is a promising tool for detecting early SCC lesions of the skin. Pretreatment with VD can increase the ability to detect early tumors, providing a potential new way to improve efficacy of ALA-PDT.
机译:在皮肤的鳞状细胞癌(SCC)的光动力疗法(PDT)之前和期间,需要更好的无创技术来监测原卟啉IX(PpIX)的水平。我们的目的是评估:(1)在SCC小鼠模型中对紫外线(UV)诱发的癌症和癌前病变进行多光谱荧光成像; (2)多光谱成像和基于探针的荧光检测作为研究维生素D(VD)对氨基乙酰丙酸(ALA)诱导的PpIX合成的作用的工具。在24周的紫外线致癌方案中,每周对无毛小鼠的背部皮肤进行成像。在暴露于紫外线的14周后,可以通过多光谱成像检测到PpIX荧光的热点。在第20周停止紫外线后,许多热点消失了,但是在第20周之后,其他热点仍然存在或变得可见,并且对应于最终被肉眼看到的肿瘤。在使用ALA之前使用局部VD预处理的荷SCC小鼠中,我们的光学技术证实了VD预处理可诱导肿瘤选择性PpIX水平升高。 PpIX的基于荧光的光学成像是检测皮肤早期SCC病变的有前途的工具。 VD预处理可以提高发现早期肿瘤的能力,为提高ALA-PDT的疗效提供了一种潜在的新途径。

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