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Enhancing protoporphyrin IX-induced PDT

机译:增强原因卟啉IX诱导的PDT

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Photodynamic therapy (PDT) using porphyrin precursors is commonly used in dermatology. Evidence indicates that good clinical outcomes (associated with excellent cosmesis) can be achieved in superficial precancers and basal cell carcinoma (BCC), however, efficacy appears less favorable for thicker nodular BCC (nBCC) unless multiple PDT treatment cycles are performed. Enhancement is therefore required if nBCC lesions are to be treated effectively with a single PDT treatment. The most common technique currently being routinely employed clinically is the use of aminolevulinic acid (ALA) esters (usually methyl (MAL) or hexyl (HAL)). Standard dermatological PDT employing these porphyrin precursors already manipulates the normal heme biosynthesis pathway resulting in a temporary accumulation of the natural photosensitizer, protoporphyrin IX (PpIX). Further manipulation using iron chelating agents is possible however. In normal and malignant human cells in vitro, the novel iron chelating agent CP94 produced greater PPIX fluorescence when administered with ALA or MAL than either congener produced alone. CP94 was also significantly more effective than the clinically established iron chelating agent desferrioxamine (DFO). Topical application of ALA+CP94 to clinical nBCC lesions was a simple and safe treatment modification which produced a significant increase in clinical clearance when CP94 was included in the cream.
机译:使用卟啉前体的光动力治疗(PDT)通常用于皮肤科。证据表明,除非进行多种PDT治疗循环,否则良好的临床结果(与良好的患者相关)可以在浅表血糖和基础细胞癌(BCC)中实现较厚的结节BCC(NBCC)。因此,如果用单个PDT处理有效地治疗NBCC病变,则需要增强。目前临床上常规使用的最常用技术是使用氨基乙酰丙烯酸(ALA)酯(通常是甲基(MAL)或己基(HAL))。使用这些卟啉前体的标准皮肤病学PDT已经操纵了正常血红素生物合成途径,导致自然光敏剂,原子卟啉IX(PPIX)临时积累。然而,使用铁螯合剂的进一步操纵也是可能的。在体外的正常和恶性人体细胞中,新颖的铁螯合剂CP94在用Ala或Malm施用时产生更大的ppix荧光,而不是单独制备的链烷物。 CP94也比临床成立的铁螯合剂除氟甲胺(DFO)更有效。 ALA + CP94至临床NBCC病变的局部应用是一种简单且安全的处理改性,当CP94包含在乳膏中时,临床间隙的显着增加。

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