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糖基树枝状苯卟啉作为视网膜母细胞瘤光动力疗法的新候选物:血液载体和细胞中的光动力活性。

Glycodendrimeric phenylporphyrins as new candidates for retinoblastoma PDT: blood carriers and photodynamic activity in cells.

机构信息

EA 4041, Laboratoire de Chimie Analytique, IFR 141, Univ. Paris-Sud, 5 rue J.-B. Clément, F-92296 Châtenay-Malabry, France.

出版信息

J Photochem Photobiol B. 2012 Oct 3;115:16-24. doi: 10.1016/j.jphotobiol.2012.06.005. Epub 2012 Jun 19.

DOI:10.1016/j.jphotobiol.2012.06.005
PMID:22796430
Abstract

Photodynamic therapy (PDT) has recently been proposed as a possible indication in the conservative treatment of hereditary retinoblastoma. In order to create photosensitizers with enhanced targeting ability toward retinoblastoma cells, meso-tetraphenylporphyrins bearing one glycodendrimeric moiety have been synthesized. The binding properties to plasma proteins and photodynamic activity of two monodendrimeric porphyrins bearing three mannose units via monoethylene glycol (1) or diethylene glycol (2) linkers have been compared to that of the non-dendrimeric tri-substituted derivative [TPP(p-Deg-O-α-ManOH)(3)]. The dendrimeric structure was found to highly increase the binding affinity to plasma proteins and to modify to some extent plasma distribution. HDL and to a lesser extent LDL have been shown to be the main carriers of dendrimeric and non-dendrimeric compounds. The phototoxicity observed for the two glycodendrimers (1) and (2) (LD(50)=0.5 μM) in Y79 cells is of the same order of magnitude that for TPP(p-Deg-O-α-ManOH)(3) (LD(50)=0.7 μM), with a similar cellular uptake level for (1) and a lower for (2). A serum content increase from 2% to 20% (v/v) in the incubation medium was found to inhibit both cellular uptake and photoactivity of dendrimeric derivatives, whereas those of TPP(p-Deg-O-α-ManOH)(3) remained little affected. Specificities of glycodendrimeric porphyrins, combining a lower cellular uptake together with a higher affinity toward plasma proteins, make these derivatives possible candidates for a vascular targeting PDT.

摘要

光动力疗法(PDT)最近被提议作为遗传性视网膜母细胞瘤保守治疗的一种可能选择。为了制备对视网膜母细胞瘤细胞具有增强靶向能力的光敏剂,已经合成了带有一个糖基树枝状大分子部分的中位四苯基卟啉。通过单乙二醇(1)或二乙二醇(2)接头带有三个甘露糖单元的两个单树枝状卟啉的结合特性对血浆蛋白和光动力活性与非树枝状三取代衍生物[TPP(p-Deg-O-α-ManOH)(3)]进行了比较。研究发现树枝状结构高度增加了与血浆蛋白的结合亲和力,并在某种程度上改变了血浆分布。已经表明,HDL 和 LDL 在一定程度上是树枝状和非树枝状化合物的主要载体。在 Y79 细胞中观察到的两种糖基树枝状聚合物(1)和(2)(LD50=0.5 μM)的光毒性与 TPP(p-Deg-O-α-ManOH)(3)(LD50=0.7 μM)相当,(1)的细胞摄取水平相似,而(2)的细胞摄取水平较低。在孵育培养基中血清含量从 2%增加到 20%(v/v)时,发现树枝状衍生物的细胞摄取和光活性均受到抑制,而 TPP(p-Deg-O-α-ManOH)(3)的光活性几乎不受影响。糖基树枝状卟啉的特异性结合了较低的细胞摄取和对血浆蛋白的较高亲和力,使得这些衍生物成为血管靶向 PDT 的候选药物。

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