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与紫红素亚胺相比,含有碘苄基的焦脱镁叶绿酸表现出增强的光动力疗法(PDT)疗效和肿瘤成像(124I-PET)能力。

Compared to purpurinimides, the pyropheophorbide containing an iodobenzyl group showed enhanced PDT efficacy and tumor imaging (124I-PET) ability.

作者信息

Pandey Suresh K, Sajjad Munawwar, Chen Yihui, Pandey Anupam, Missert Joseph R, Batt Carrie, Yao Rutao, Nabi Hani A, Oseroff Allan R, Pandey Ravindra K

机构信息

PDT Center, Cell Stress Biology and Department of Dermatology, Roswell Park Cancer Institute, Buffalo, New York 14263, USA.

出版信息

Bioconjug Chem. 2009 Feb;20(2):274-82. doi: 10.1021/bc8003638.

Abstract

Two positional isomers of purpurinimide, 3-[1'-(3-iodobenzyloxyethyl)] purpurin-18-N-hexylimide methyl ester 4, in which the iodobenzyl group is present at the top half of the molecule (position-3), and a 3-(1'-hexyloxyethy)purpurin-18-N-(3-iodo-benzylimide)] methyl ester 5, where the iodobenzyl group is introduced at the bottom half (N-substitued cyclicimide) of the molecule, were derived from chlorophyll-a. The tumor uptake and phototherapeutic abilities of these isomers were compared with the pyropheophorbide analogue 1 (lead compound). These compounds were then converted into the corresponding 124I-labeled PET imaging agents with specific activity >1 Ci/micromol. Among the positional isomers 4 and 5, purpurinimide 5 showed enhanced imaging and therapeutic potential. However, the lead compound 1 derived from pyropheophorbide-a exhibited the best PET imaging and PDT efficacy. For investigating the overall lipophilicity of the molecule, the 3-O-hexyl ether group present at position-3 of purpurinimide 5 was replaced with a methyl ether substituent, and the resulting product 10 showed improved tumor uptake, but due to its significantly higher uptake in the liver, spleen, and other organs, a poor tumor contrast in whole-body tumor imaging was observed.

摘要

紫红素-18-亚胺的两种位置异构体,即3-[1'-(3-碘苄氧基乙基)]紫红素-18-N-己基亚胺甲酯4(其中碘苄基位于分子的上半部分(3位))和3-(1'-己氧基乙基)紫红素-18-N-(3-碘苄基亚胺)]甲酯5(其中碘苄基引入到分子的下半部分(N-取代的环亚胺)),是由叶绿素-a衍生而来的。将这些异构体的肿瘤摄取和光治疗能力与焦脱镁叶绿酸类似物1(先导化合物)进行了比较。然后将这些化合物转化为比活度>1 Ci/μmol的相应124I标记的PET显像剂。在位置异构体4和5中,紫红素-18-亚胺5显示出增强的显像和治疗潜力。然而,由焦脱镁叶绿酸-a衍生的先导化合物1表现出最佳的PET显像和光动力治疗效果。为了研究分子的整体亲脂性,将紫红素-18-亚胺5的3位上存在的3-O-己基醚基团替换为甲醚取代基,所得产物10显示出改善的肿瘤摄取,但由于其在肝脏、脾脏和其他器官中的摄取显著更高,在全身肿瘤显像中观察到较差的肿瘤对比度。

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