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Enhancement of 5-aminolaevulinic acid-induced photodynamic therapy in normal rat colon using hydroxypyridinone iron-chelating agents

机译:羟基吡啶酮铁螯合剂增强5-氨基戊酸对正常大鼠结肠的光动力治疗

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Currently, the clinical use of 5-aminolaevulinic acid (ALA)-induced protoporphyrin IX (PPIX) for photodynamic therapy (PDT) is limited by the maximum tolerated oral ALA dose (60 mg kg(-1)). This study investigates whether hydroxypyridinone iron-chelating agents can be used to enhance the tissue levels of PPIX, without increasing the administered dose of ALA. Quantitative charge-coupled device (CCD) fluorescence microscopy was employed to study PPIX fluorescence pharmacokinetics in the colon of normal Wistar rats. The iron chelator, CP94, when administered with ALA was found to produce double the PPIX fluorescence in the colonic mucosa, compared with the same dose of ALA given alone and to be more effective than the other iron chelator studied, CP20. Microspectrofluorimetric studies demonstrated that PPIX was the predominant porphyrin species present. PDT studies conducted on the colonic mucosa showed that the simultaneous administration of 100 mg kg(-1) CP94 i.v. and 50 mg kg(-1) ALA i.v. produced an area of necrosis three times larger than similar parameters without the iron-chelating agent with the same light dose. It is possible, therefore, to increase the amount of necrosis produced by ALA-induced PDT substantially, without increasing the administered dose of ALA, through the simultaneous administration of the iron-chelating agent, CP94.
机译:当前,5-氨基松香酸(ALA)诱导的原卟啉IX(PPIX)在光动力疗法(PDT)中的临床使用受到最大耐受口服ALA剂量(60 mg kg(-1))的限制。这项研究调查了羟基吡啶酮铁螯合剂是否可用于增强PPIX的组织水平,而不增加ALA的给药剂量。定量电荷耦合器件(CCD)荧光显微镜用于研究正常Wistar大鼠结肠中PPIX荧光的药代动力学。与单独使用相同剂量的ALA相比,铁螯合剂CP94与ALA一起使用时,在结肠粘膜中产生的PPIX荧光增加了一倍,并且比其他研究的铁螯合剂CP20更有效。显微荧光光谱分析表明,PPIX是目前存在的主要卟啉物质。对结肠粘膜进行的PDT研究表明,同时给予100 mg kg(-1)CP94 i.v.和50 mg kg(-1)ALA i.v.在没有相同剂量的铁螯合剂的情况下,产生的坏死面积是类似参数的三倍。因此,通过同时施用铁螯合剂CP94,可以在实质上不增加ALA的给药剂量的情况下,增加ALA诱导的PDT产生的坏死的数量。

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