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Potentiation of ALA-PDT antitumor activity in mice using topical DMXAA

机译:使用局部DMXAA的小鼠中ALA-PDT抗肿瘤活性的增强

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Photodynamic treatment of subcutaneously implanted Colon 26 tumors in BALB/c mice using the aminolevulinic acid (ALA)-induced photosensitizer protoporphyrin IX (PpIX) was shown to be enhanced by the addition of the vascular disrupting agent 5,6-Dimethylxanthenone-4-acetic-acid (DMXAA; Novartis ASA404). DMXAA increases vascular permeability and decreases blood flow in both murine and human tumors. Sufficiently high parenteral DMXAA doses can lead to tumor collapse and necrosis. We have previously reported marked enhancement of antitumor activity when PDT, using either Photofrin or HPPH, is combined with low-dose intraperitoneal DMXAA. We now describe the first attempt to combine topically-applied DMXAA with PDT. For this, DMXAA was applied two hours before PpIX-activating light delivery. PDT with ALA-PDT alone (ALA 20%; 80 J/cm~2 delivered at 75 mW/cm~2) caused a 39% decrease in tumor volume compared to unirradiated controls. Addition of topical DMXAA to ALA-PDT resulted in a 74% reduction in tumor volume. Diffuse correlation spectroscopy (DCS), a non-invasive blood flow imaging method, is being used to understand the mechanism of this effect and to aid in the proper design of the therapy. For instance, our most recent DCS data suggests that the 2-hour interval between the DMXAA and light applications may not be optimum. This preliminary study suggests a potential role for topical DMXAA in combination with PDT for dermatologic tumors.
机译:在BALB皮下植入结肠26个肿瘤的光动力治疗/使用氨基乙酰丙酸(ALA)c小鼠诱导的原卟啉光敏剂啉IX(PpIX)显示出通过加入血管破坏剂5,6-二甲基呫吨-4-乙酸来增强 - 酸(DMXAA;诺华ASA404)。 DMXAA增加血管渗透性,并且降低在鼠和人类肿瘤的血流。足够高的注射剂量的DMXAA导致肿瘤塌陷,坏死。当PDT,即使用光敏素或HPPH我们曾报道明显强化的抗肿瘤活性,与低剂量腹腔DMXAA组合。我们现在描述的第一次尝试,以局部应用DMXAA与PDT结合。对于这一点,DMXAA是前两小时的PpIX激活光递送施用。 PDT单独使用ALA-PDT(ALA 20%; 80焦耳/平方厘米〜2在75毫瓦/平方厘米〜2传送)造成的肿瘤体积的39%相比,减少未经照射的对照。局部DMXAA到ALA-PDT的加入导致在肿瘤体积减少74%。漫相关光谱法(DCS),非侵入性的血流成像方法,被用于了解这种作用的机制和治疗的适当的设计,以帮助。例如,我们最近的数据DCS表明DMXAA和光应用程序之间的2小时的时间间隔可能不是最佳的。这一初步研究表明局部DMXAA结合PDT用于皮肤病肿瘤的潜在作用。

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