首页> 外文期刊>British Journal of Cancer >A comparative study of tissue distribution and photodynamic therapy selectivity of chlorin e6, Photofrin II and ALA-induced protoporphyrin IX in a colon carcinoma model
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A comparative study of tissue distribution and photodynamic therapy selectivity of chlorin e6, Photofrin II and ALA-induced protoporphyrin IX in a colon carcinoma model

机译:二氢卟酚e6,Photofrin II和ALA诱导的原卟啉IX在结肠癌模型中的组织分布和光动力疗法选择性的比较研究

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An in vivo study of tissue distribution kinetics and photodynamic therapy (PDT) using 5-aminolaevulinic acid (ALA), chlorin e6 (Chl) and Photofrin (PII) was performed to evaluate the selectivity of porphyrin accumulation and tissue damage effects in a tumour model compared with normal tissue. C26 colon carcinoma of mice transplanted to the foot was used as a model for selectivity assessment. Fluorescence measurements of porphyrin accumulation in the foot bearing the tumour and in the normal foot were performed by the laser-induced fluorescence (LIF) system. A new high-intensity pulsed light delivery system (HIPLS) was used for simultaneous irradiation of both feet by light in the range of 600-800 nm, with light doses from 120 to 300 J cm-2 (0.6 J cm-2 per pulse, 1 Hz). Photoirradiation was carried out 1 h after injection of ALA, 3 h after injection of Chl and 24 h after injection of PII. A ratio of porphyrin accumulation in tumour vs normal tissue was used as an index of accumulation selectivity for each agent. PDT selectivity was determined from the regression analysis of normal and tumour tissue responses to PDT as a function of the applied light dose. A normal tissue damage index was defined at various values (50, 80 and 100%) of antitumour effect. The results of the LIF measurements revealed different patterns of fluorescence intensity in tumour and normal tissues for ALA-induced protoporphyrin IX (ALA-PpIX), Chl and PII. The results of PDT demonstrated the differences in both anti-tumour efficiency and normal tissue damage for the agents used. The selectivity of porphyrin accumulation in the tumour at the time of photoirradiation, as obtained by the LIF measurements, was in the order ALA-PpIX > Chl > PII. PDT selectivity at an equal value of anti-tumour effect was in the order Chl > ALA-PpIX > PII. Histological examination revealed certain differences in structural changes of normal skin after PDT with the agents tested. The results of PDT selectivity assessment with respect to differences in mechanisms of action for ALA, Chl and PII are discussed.
机译:进行了体内分布动力学和光动力疗法(PDT)的体内研究,该疗法使用5-氨基松香酸(ALA),二氢卟酚e6(Chl)和Photofrin(PII)评估了卟啉积聚的选择性以及组织在肿瘤模型中的损伤作用与正常组织相比。将移植到脚的小鼠的C26结肠癌用作选择性评估的模型。用激光诱导荧光(LIF)系统进行卟啉在肿瘤足和正常足中积累的荧光测量。使用新的高强度脉冲光传输系统(HIPLS),以600-800 nm范围内的光同时照射双脚,光剂量为120至300 J cm-2(每个脉冲0.6 J cm-2 ,1 Hz)。注射ALA后1小时,注射Chl后3小时和注射PII后24小时进行光照射。肿瘤与正常组织中卟啉积累的比率用作每种药剂的积累选择性的指标。根据正常和肿瘤组织对PDT的反应的回归分析确定PDT的选择性,作为对所施加光剂量的函数。正常组织损伤指数定义为抗肿瘤作用的各种值(50%,80%和100%)。 LIF测量的结果显示,ALA诱导的原卟啉IX(ALA-PpIX),Chl和PII在肿瘤和正常组织中的荧光强度不同。 PDT的结果证明了所用药物在抗肿瘤效率和正常组织损伤方面均存在差异。通过LIF测量获得的在光照射时卟啉在肿瘤中积累的选择性为ALA-PpIX> Chl> PII。在相等的抗肿瘤作用值下,PDT的选择性依次为Chl> ALA-PpIX> PII。组织学检查显示,PDT与受试药物后,正常皮肤的结构变化存在一定差异。讨论了有关ALA,Chl和PII作用机理差异的PDT选择性评估结果。

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