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Photodynamic therapy effect of m-THPC (Foscan|[reg]|) in vivo: correlation with pharmacokinetics

机译:m-THPC(Foscan | [reg] |)在体内的光动力治疗作用:与药代动力学的关系

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m-Tetra(hydroxyphenyl)chlorin (m-THPC, Foscan, Temoporfin) has an unusually high photodynamic efficacy which cannot be explained by its photochemical properties alone. In vivo interactions are therefore of critical importance in determining this high potency. The pharmacokinetics of m-THPC in a rat tumour model was determined using 14C m-THPC in an LSBD1 fibrosarcoma implanted into BDIX rats. The photodynamic therapy (PDT) efficacy was determined at different drug administrations to light intervals and correlated with the tumour and plasma pharmacokinetic data. The plasma pharmacokinetics of m-THPC can be interpreted by compartmental analysis as having three half-lives of 0.46, 6.91 and 82.5?h, with a small initial volume of distribution, suggesting retention in the vascular compartment. Tissues of the reticuloendothelial system showed high accumulation of m-THPC, particularly the liver. PDT efficacy of m-THPC over the same time course seemed to exhibit two peaks of activity (2 and 24?h), in terms of tumour growth delay with the peak at 24?h postinjection correlating to the maximum tumour concentration. Investigation on tumour cells isolated from m-THPC-treated tumours suggested that the peak PDT activity at 2?h represents an effect on the vasculature while the peak at 24?h shows a more direct response. These results indicate that the in vivo PDT effect of m-THPC occurs via several mechanisms.
机译:间四(羟苯基)二氢卟酚(m-THPC,Foscan,替莫泊芬)具有异常高的光动力功效,仅凭其光化学性质无法解释。因此,体内相互作用对于确定这种高效力至关重要。使用14 C m-THPC在植入BDIX大鼠的LSBD1纤维肉瘤中确定m-THPC在大鼠肿瘤模型中的药代动力学。在不同的给药间隔下确定光动力疗法(PDT)的疗效,并与肿瘤和血浆药代动力学数据相关。 m-THPC的血浆药代动力学可以通过隔室分析解释为具有三个半衰期,分别为0.46、6.91和82.5?h,初始分布量较小,表明保留在血管室中。网状内皮系统的组织显示出m-THPC的高积累,尤其是肝脏。就肿瘤生长延迟而言,m-THPC在同一时间过程中的PDT功效似乎表现出两个活性峰(2和24?h),而注射后24?h的峰与最大肿瘤浓度相关。对从经m-THPC处理的肿瘤中分离的肿瘤细胞进行的研究表明,PDT活性在2?h时的峰值代表对脉管系统的影响,而24?h处的峰值则表现出更直接的反应。这些结果表明,m-THPC的体内PDT作用通过几种机制发生。

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