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新型潜在多巴胺转运体示踪剂[18F]FE@CIT的合成与生物分布

Synthesis and biodistribution of [18F]FE@CIT, a new potential tracer for the dopamine transporter.

作者信息

Mitterhauser Markus, Wadsak Wolfgang, Mien Leonhard-Key, Hoepping Alexander, Viernstein Helmut, Dudczak Robert, Kletter Kurt

机构信息

Department of Nuclear Medicine, Medical University of Vienna, Austria.

出版信息

Synapse. 2005 Feb;55(2):73-9. doi: 10.1002/syn.20095.

DOI:10.1002/syn.20095
PMID:15529336
Abstract

In the last decade radiolabeled tropane analogs based on beta-CIT have proven indispensable for the imaging of the dopamine transporter. However, further improvements in their pharmacodynamic and pharmacokinetic features are desirable. An important improvement, yielding in higher affinity to the dopamine transporter (DAT) vs. serotonin transporter (SERT), can be achieved by a simple replacement of the carboxylic methyl ester group in beta-CIT by a fluoroethyl ester. The preparation and ex vivo evaluation of this new beta-CIT-analog ([18F]FE@CIT) is presented here. Precursor and standard were prepared from beta-CIT and analyzed by spectroscopic methods. Yields of precursor and standard preparation were 61% and 42%, respectively. [18F]FE@CIT was prepared by distillation of [18F]bromofluoroethane ([18F]BFE) and reaction with (1R-2-exo-3-exo)8-methyl-3-(4-iodo-phenyl)-8-azabicyclo[3.2.1] octane-2-carboxylic acid. After 10 min at 150 degrees C the product was purified using a C-18 SepPak. The radiosynthesis evinced radiochemical yields of >90% (based on [18F]BFE), the specific radioactivity was >416 GBq/micromol. An average 30 microAh cyclotron irradiation yielded more than 2.5 GBq [18F]FE@CIT. For the ex vivo bioevaluation, 20 male Sprague-Dawley rats were sacrificed at 5, 15, 30, 60, and 120 min after injection. Organs were removed, weighed, and counted. For autoradiographic experiments, transverse brain slices of about 100 microm were prepared. The ex vivo evaluation showed highest brain uptake in striatal regions, followed by thalamus and cerebellum. The highest striatum to cerebellum ratio was 3.73 and the highest thalamus to cerebellum ratio was 1.65. Autoradiographic images showed a good and differentiated uptake in striatal regions with a good target-to-background ratio.

摘要

在过去十年中,基于β-CIT的放射性标记托烷类似物已被证明在多巴胺转运体成像中不可或缺。然而,其药效学和药代动力学特性仍有待进一步改善。通过将β-CIT中的羧酸甲酯基团简单替换为氟乙酯,可以实现对多巴胺转运体(DAT)相对于5-羟色胺转运体(SERT)更高的亲和力这一重要改进。本文介绍了这种新型β-CIT类似物([18F]FE@CIT)的制备及体外评估。前体和标准品由β-CIT制备,并通过光谱方法进行分析。前体和标准品制备的产率分别为61%和42%。[18F]FE@CIT通过蒸馏[18F]溴氟乙烷([18F]BFE)并与(1R-2-exo-3-exo)8-甲基-3-(4-碘苯基)-8-氮杂双环[3.2.1]辛烷-2-羧酸反应制备。在150℃下反应10分钟后,使用C-18 SepPak对产物进行纯化。放射合成显示放射化学产率>90%(基于[18F]BFE),比活度>416 GBq/μmol。平均30微安的回旋加速器辐照产生了超过2.5 GBq的[18F]FE@CIT。为进行体外生物评估,在注射后5分钟至120分钟的不同时间点处死20只雄性Sprague-Dawley大鼠。取出器官,称重并计数。进行放射自显影实验时,制备了约100微米厚的脑横切片。体外评估显示纹状体区域的脑摄取最高,其次是丘脑和小脑。纹状体与小脑的最高比值为3.73,丘脑与小脑的最高比值为1.65。放射自显影图像显示纹状体区域摄取良好且有差异,靶本底比值良好。

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