光动力疗法中各种光敏剂光产物对小鼠迟发性超敏反应的调节作用。

Alla A Kyagova, Ludmila A Kozir, Galina V Mansurova, Vladimir P Zorin, Lina N Bezdetnaya, Fracoise Guillemin, Alexander Ya Potapenko
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引用次数: 0

摘要

光动力疗法经常伴随着免疫抑制的诱导。诱导这种免疫抑制的光化学机制尚不清楚。本研究的目的是评估merocyanine 540 (MC540)、protoporphyrin IX (PPIX)和hematporphyrin衍生物(HpD)的光产物在体内引起T细胞免疫反应调节(抑制/激活)的潜力。我们采用的方法是光敏剂溶液的预照射,随后将光敏剂光降解产物应用于动物。在这种方法中,I型和II型的光化学机制不涉及体内生物靶点的光敏修饰。利用小鼠对绵羊红细胞的延迟型超敏反应(DTH)模型,我们证明了三种本质上不同的光敏剂的光产物影响t细胞免疫。HpD光降解产物对DTH有抑制作用,而PPIX光降解产物对DTH有近2倍的增强作用。预照射MC540能强烈调节DTH反应,即低剂量时DTH增强,高剂量时DTH抑制。我们的研究结果强烈表明,至少部分光动力疗法诱导的免疫调节可能是通过光敏剂的光漂白伴随光产物的产生而发生的,这可以影响T细胞的免疫。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Modulation of delayed type hypersensitivity in mice treated with photoproducts of various photosensitizers used in photodynamic therapy.

Photodynamic therapy is frequently accompanied by the induction of immunosuppression. The photochemical mechanisms behind the induction of this immunosuppression are not clear. The purpose of this study was to evaluate the potential of photoproducts of merocyanine 540 (MC540), protoporphyrin IX (PPIX) and hematoporphyrin derivative (HpD) to cause modulation (suppression/activation) of the T cell immune response in vivo. The approach that we have adopted is the pre-irradiation of a photosensitizer solution with the subsequent application of the products of photosensitizer photodegradation in animals. In this approach the photochemical mechanisms of type I and II are not involved in the photosensitized modification of biological targets in vivo. Using the model of delayed type hypersensitivity (DTH) reaction to sheep red blood cells in mice, we have demonstrated that the photoproducts of three essentially different photosensitizers affect T-cell immunity. The HpD photoproducts had a suppressive effect on the DTH, while products of PPIX photodegradation enhanced the DTH nearly twice. Pre-irradiated MC540 strongly modulated the DTH response, i.e. the DTH was enhanced at low doses and inhibited at higher doses. Our results strongly indicate that at least part of the photodynamic therapy-induced immunomodulation may occur via the photobleaching of photosensitizers accompanied by the generation of photoproducts, which can affect T cell immunity.

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