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Photoproducts of the Photodynamic Therapy Agent Verteporfin Identified via Laser Interfaced Mass Spectrometry

机译:通过激光接口质谱法鉴定的光动力治疗剂的光调节素

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摘要

Verteporfin, a free base benzoporphyrin derivative monoacid ring A, is a photosensitizing drug for photodynamic therapy (PDT) used in the treatment of the wet form of macular degeneration and activated by red light of 689 nm. Here, we present the first direct study of its photofragmentation channels in the gas phase, conducted using a laser interfaced mass spectrometer across a broad photoexcitation range from 250 to 790 nm. The photofragmentation channels are compared with the collision-induced dissociation (CID) products revealing similar dissociation pathways characterized by the loss of the carboxyl and ester groups. Complementary solution-phase photolysis experiments indicate that photobleaching occurs in verteporfin in acetonitrile; a notable conclusion, as photoinduced activity in Verteporfin was not thought to occur in homogenous solvent conditions. These results provide unique new information on the thermal break-down products and photoproducts of this light-triggered drug.
机译:RESTEPORFIN,一种游离碱苯并卟啉衍生物单酸环A,是用于光动力治疗(PDT)的光敏药物,用于治疗湿式变性的湿式变性,并通过689nm的红光激活。这里,我们介绍了在气相中使用激光接口质谱仪在气相中进行的第一次直接研究,横跨250至790nm的广泛的光筛选。将光碎片沉积通道与露天诱导的解离(CID)产品进行比较,揭示了具有羧基和酯基的损失的相似解离途径。互补溶液相光解实验表明光漂白在乙腈中的verteporfin中发生;值得注意的结论是由于在均匀的溶剂条件下未被认为在甲状腺素中的光诱导活性。这些结果提供了关于这种光触发药物的热分解产品和光调节的独特新信息。

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