The Search for a Subtype-Selective PET Imaging Agent for the GABAA Receptor Complex: Evaluation of the Radiotracer [11C]ADO in Nonhuman Primates.

IF 2.2 4区 医学 Q3 BIOCHEMICAL RESEARCH METHODS Molecular Imaging Pub Date : 2017-01-01 DOI:10.1177/1536012117731258
Shu-Fei Lin, Frederic Bois, Daniel Holden, Nabeel Nabulsi, Richard Pracitto, Hong Gao, Michael Kapinos, Jo-Ku Teng, Anupama Shirali, Jim Ropchan, Richard E Carson, Charles S Elmore, Neil Vasdev, Yiyun Huang
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引用次数: 8

Abstract

The myriad physiological functions of γ-amino butyric acid (GABA) are mediated by the GABA-benzodiazepine receptor complex comprising of the GABAA, GABAB, and GABAC groups. The various GABAA subunits with region-specific distributions in the brain subserve different functional and physiological roles. For example, the sedative and anticonvulsive effects of classical benzodiazepines are attributed to the α1 subunit, and the α2 and α3 subunits mediate the anxiolytic effect. To optimize pharmacotherapies with improved efficacy and devoid of undesirable side effects for the treatment of anxiety disorders, subtype-selective imaging radiotracers are required to assess target engagement at GABA sites and determine the dose-receptor occupancy relationships. The goal of this work was to characterize, in nonhuman primates, the in vivo binding profile of a novel positron emission tomography (PET) radiotracer, [11C]ADO, which has been indicated to have functional selectivity for the GABAA α23 subunits. High specific activity [11C]ADO was administrated to 3 rhesus monkeys, and PET scans of 120-minute duration were performed on the Focus-220 scanner. In the blood, [11C]ADO metabolized at a fairly rapid rate, with ∼36% of the parent tracer remaining at 30 minutes postinjection. Uptake levels of [11C]ADO in the brain were high (peak standardized uptake value of ∼3.0) and consistent with GABAA distribution, with highest activity levels in cortical areas, intermediate levels in cerebellum and thalamus, and lowest uptake in striatal regions and amygdala. Tissue kinetics was fast, with peak uptake in all brain regions within 20 minutes of tracer injection. The one-tissue compartment model provided good fits to regional time-activity curves and reliable measurement of kinetic parameters. The absolute test-retest variability of regional distribution volumes ( VT) was low, ranging from 4.5% to 8.7%. Pretreatment with flumazenil (a subtype nonselective ligand, 0.2 mg/kg, intravenous [IV], n = 1), Ro15-4513 (an α5-selective ligand, 0.03 mg/kg, IV, n = 2), and zolpidem (an α1-selective ligand, 1.7 mg/kg, IV, n = 1) led to blockade of [11C]ADO binding by 96.5%, 52.5%, and 76.5%, respectively, indicating the in vivo binding specificity of the radiotracer. Using the nondisplaceable volume of distribution ( VND) determined from the blocking studies, specific binding signals, as measured by values of regional binding potential ( BPND), ranged from 0.6 to 4.4, which are comparable to those of [11C]flumazenil. In conclusion, [11C]ADO was demonstrated to be a specific radiotracer for the GABAA receptors with several favorable properties: high brain uptake, fast tissue kinetics, and high levels of specific binding in nonhuman primates. However, subtype selectivity in vivo is not obvious for the radiotracer, and thus, the search for subtype-selective GABAA radiotracers continues.

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寻找GABAA受体复合物亚型选择性PET显像剂:对非人灵长类动物放射性示踪剂[11C]ADO的评价。
γ-氨基丁酸(GABA)的多种生理功能是由GABAA、GABAB和GABAC基团组成的GABA-苯二氮卓类受体复合物介导的。GABAA亚基在大脑中具有区域特异性分布,具有不同的功能和生理作用。例如,经典苯二氮卓类药物的镇静和抗惊厥作用归因于α1亚基,α2和α3亚基介导抗焦虑作用。为了优化药物治疗,提高疗效,消除不良副作用,治疗焦虑症,需要亚型选择性成像放射性示踪剂来评估GABA位点的靶标参与,并确定剂量-受体占用关系。这项工作的目的是在非人灵长类动物中表征一种新型正电子发射断层扫描(PET)放射性示踪剂[11C]ADO的体内结合谱,该示踪剂已被证明对GABAA α2/α3亚基具有功能选择性。给3只恒河猴注射高比活性[11C]ADO,在Focus-220扫描仪上进行持续120分钟的PET扫描。在血液中,[11C]ADO代谢速度相当快,注射后30分钟仍有36%的母体示踪剂残留。大脑中[11C]ADO的摄取水平很高(峰值标准化摄取值为3.0),与GABAA分布一致,皮质区活动水平最高,小脑和丘脑处于中等水平,纹状体区和杏仁核的摄取最低。组织动力学很快,在注射示踪剂20分钟内,所有脑区都有峰值摄取。单组织室模型对区域时间-活性曲线拟合良好,动力学参数测量可靠。区域分布体积(VT)的绝对重测变异性较低,在4.5% ~ 8.7%之间。氟马西尼(一种亚型非选择性配体,0.2 mg/kg,静脉注射[IV], n = 1)、Ro15-4513(一种α5选择性配体,0.03 mg/kg,静脉注射,n = 2)和唑吡坦(一种α1选择性配体,1.7 mg/kg,静脉注射,n = 1)预处理对[11C]ADO结合的阻断率分别为96.5%、52.5%和76.5%,表明放射性示踪剂的体内结合特异性。使用从阻断研究中确定的不可置换分布体积(VND),通过区域结合电位(BPND)值测量的特异性结合信号范围为0.6至4.4,与[11C]氟马西尼相当。总之,[11C]ADO被证明是GABAA受体的特异性放射性示踪剂,在非人灵长类动物中具有几个有利的特性:高脑摄取、快速组织动力学和高水平的特异性结合。然而,放射性示踪剂在体内的亚型选择性并不明显,因此,对亚型选择性GABAA放射性示踪剂的研究仍在继续。
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来源期刊
Molecular Imaging
Molecular Imaging Biochemistry, Genetics and Molecular Biology-Biotechnology
自引率
3.60%
发文量
21
期刊介绍: Molecular Imaging is a peer-reviewed, open access journal highlighting the breadth of molecular imaging research from basic science to preclinical studies to human applications. This serves both the scientific and clinical communities by disseminating novel results and concepts relevant to the biological study of normal and disease processes in both basic and translational studies ranging from mice to humans.
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