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14C标记的间四羟基苯基二氢卟酚和5-氨基乙酰丙酸在C6大鼠胶质瘤模型中的摄取与动力学

Uptake and kinetics of 14C-labelled meta-tetrahydroxyphenylchlorin and 5-aminolaevulinic acid in the C6 rat glioma model.

作者信息

Obwegeser A, Jakober R, Kostron H

机构信息

Department of Neurosurgery, University of Innsbruck, Austria.

出版信息

Br J Cancer. 1998 Sep;78(6):733-8. doi: 10.1038/bjc.1998.569.

Abstract

Meta-tetrahydroxyphenylchlorin (m-THPC) and 5-aminolaevulinic acid (5-ALA) are two second-generation photosensitizers which are currently under investigation for photodynamic therapy (PDT) and photodynamic diagnosis (PDD). So far, the experience with these photosensitizers for use within brain tumours is limited. We examined the distribution and retention of 14C-labelled m-THPC and [14C]5-ALA in the rat C6 glioma brain tumour model. After intraperitoneal injection of m-THPC (71,909 d.p.m. microl(-1); 0.16 mg ml(-1) m-THPC; 0.3 mg kg(-1)), the following activities were found after 36 h: brain tumour 223,664 d.p.m. g(-1), brain contralateral to the tumour side 2567 d.p.m. g(-1), liver 369,959 d.p.m. g(-1) and skin 55,197 d.p.m. g(-1); 100,000 d.p.m. corresponding to 0.22 microg of m-THPC. After 7 days, the concentration of m-THPC decreased to 76,277 d.p.m. g(-1) in tumour and 635 d.p.m. g(-1) in brain. The radioactivity after intravenous administration of [14C]5-ALA (23,079 d.p.m. microl(-1); 40 mg ml(-1); 120 mg kg(-1)) increased within 15 min (59,634 d.p.m. g(-1) in tumour, 17,427 d.p.m. g(-1) in brain); after 8 h only a small amount (3653 d.p.m. g(-1) in tumour) remained. Brain adjacent to the tumour was also found to have a higher uptake of 5-ALA. This study provides basic information for the use of m-THPC and 5-ALA in brain tumours. Because of the different pharmacokinetic and toxicological profile, we recommend m-THPC for PDT and 5-ALA for PDD. Clinical trials now have to prove the superior phototoxic properties of these second-generation photosensitizers.

摘要

间四羟基苯基二氢卟酚(m-THPC)和5-氨基乙酰丙酸(5-ALA)是目前正在研究用于光动力疗法(PDT)和光动力诊断(PDD)的两种第二代光敏剂。到目前为止,这些光敏剂在脑肿瘤中的应用经验有限。我们在大鼠C6胶质瘤脑肿瘤模型中研究了14C标记的m-THPC和[14C]5-ALA的分布和滞留情况。腹腔注射m-THPC(71,909 衰变每分钟微升-1;0.16毫克/毫升m-THPC;0.3毫克/千克-1)后,36小时后发现以下活性:脑肿瘤223,664 衰变每分钟克-1,肿瘤对侧脑2567 衰变每分钟克-1,肝脏369,959 衰变每分钟克-1,皮肤55,197 衰变每分钟克-1;100,000 衰变每分钟相当于0.22微克的m-THPC。7天后,m-THPC在肿瘤中的浓度降至76,277 衰变每分钟克-1,在脑中降至635 衰变每分钟克-1。静脉注射[14C]5-ALA(23,079 衰变每分钟微升-1;四十毫克/毫升;120毫克/千克-1)后,15分钟内放射性增加(肿瘤中59,634 衰变每分钟克-1,脑中17,427 衰变每分钟克-1);8小时后仅残留少量(肿瘤中3653 衰变每分钟克-1)。还发现肿瘤附近的脑对5-ALA的摄取较高。本研究为m-THPC和5-ALA在脑肿瘤中的应用提供了基础信息。由于药代动力学和毒理学特征不同,我们推荐m-THPC用于PDT,5-ALA用于PDD。现在必须通过临床试验来证明这些第二代光敏剂具有更好的光毒性特性。

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