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Immune modulation using transdermal photodynamic therapy

机译:使用透皮光动力治疗免疫调节

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The photosensitizer benzoporphyrin derivative monoacid ring A (Verteporfin$+R$/ or BPD) has maximum absorption characteristics (690 nm) and biodistribution characteristics which permit activation of the drug in capillaries of the skin without causing skin photosensitivity (transdermal PDT). This permits targeting of cells in the circulation for selective ablation. Since BPD has been shown to accumulate preferentially in activated lymphocytes and monocytes, studies have been undertaken to determine the effect of transdermal PDT on murine models for rheumatoid arthritis (the MRL/lpr adjuvant enhanced model) and multiple sclerosis (the experimental allergic encephalomyelitis (EAE) model in PL mice). Localized transdermal PDT with BPD was found to be completely successful in preventing the development of adjuvant enhanced arthritis in the MRL/lpr mouse as well as improving the underlying arthritic condition of these animals. In the EAE model, in which an adoptive transfer system was used, it was found that transdermal PDT of recipients was effective in preventing EAE if treatments were implemented up to 24 hours after cell transfer but was not effective if given later, indicating the requirement for circulating T cells for effective treatment.
机译:光敏化剂苯并卟啉衍生物单酸环A(Verteporfin $ + R $ /或BPD)具有最大的吸收特性(690nm)和生物分布特征,允许在皮肤毛细管中激活药物而不会引起皮肤光敏性(透皮PDT)。这允许靶向循环中的细胞以进行选择性消融。由于已显示BPD在活性淋巴细胞和单核细胞中优先积累,因此已经进行了研究以确定透皮PDT对类风湿性关节炎(MRL / LPR佐剂增强模型)和多发性硬化症(实验性过敏脑膜炎(EAE)的鼠模型的影响)在PL小鼠中的模型)。发现具有BPD的局部透皮PDT在MRL / LPR小鼠中预防佐剂增强关节炎的发展以及改善这些动物的下面关节炎状况。在所使用的EAE模型中,在使用过养转移系统的情况下,发现如果治疗在细胞转移后24小时内实施处理,则受体的透皮PDT可有效预防EAE,但如果在后面给出,则无效,指示要求循环T细胞有效治疗。

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