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Imaging of Dopamine and Serotonin Transporters. Pre-clinical Studies with Radiotracers for Positron Emission Tomography

机译:多巴胺和5-羟色胺转运蛋白的成像。正电子发射断层扫描的放射性示踪剂的临床前研究

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摘要

The action of the neurotransmitters dopamine (DA) and serotonin (5-HT) at synapses is terminated by their rapid reuptake into presynaptic nerve endings via plasma membrane dopamine (DAT) and serotonin (SERT) transporters. Alterations in the function of these transporters have been suggested as a feature of several neurological and neuropsychiatric diseases, such as Parkinson’s disease (PD), depression, and anxiety. A suitable clinical method for studying these transporters non-invasively is positron emission tomography (PET) utilizing radiopharmaceuticals (tracers) labelled with short-lived positron-emitting radionuclides.The aim of this study was to evaluate in rats two novel radiotracers, [F]beta -CFT-FP and FFMe-McN, for imaging DAT and SERT, respectively, using , and methods. Substituting an N-methyl in [F]beta-CFT, a well known DAT tracer, with a Ffluoropropyl group significantly changed the properties of the tracer. [F]beta- CFT showed slow kinetics and metabolism, and a high specific uptake in the striatum, whereas [F]beta-CFT-FP showed fast kinetics and metabolism, and a moderate specific uptake in the striatum. [F]betaCFT-FP was selective for DAT; but [F]beta-CFT also bound to the noradrenaline transporter. [F]beta-CFT-FP may be a suitable PET tracer for imaging the striatal DAT sites, but a tracer with a higher affinity is needed for imaging extrastriatal DAT sites. In rats, FFMe-McN showed high target-to-non-target ratios, specificity and selectivity for SERT, but slow kinetics. However, FFMe-McN reveals potential for imaging SERT, at least in pre-clinical studies. In addition, the sensitivities of [F]beta CFT and [ F]FDOPA (a precursor of DA) for detecting mild nigrostriatal hypofunction were compared in an animal model of PD. The uptake of [F]FDOPA was significantly affected by compensatory effects in dopaminergic cells, whereas [F]beta-CFT was more sensitive and therefore more suitable for PET studies of mild dopaminergic symptoms.In conclusion, both novel tracers, [F]-CFT-FP and FFMe-McN, have potential, but are not optimal PET tracers for DAT and SERT imaging in rats, respectively. [F]beta-CFT is superior to [18F]FDOPA for imaging mild nigral lesions in rat brains.
机译:神经递质多巴胺(DA)和5-羟色胺(5-HT)在突触中的作用通过它们通过质膜多巴胺(DAT)和5-羟色胺(SERT)转运蛋白的快速重新摄取进入突触前神经末梢而终止。已经提出这些转运蛋白的功能改变是几种神经和神经精神疾病的特征,例如帕金森氏病(PD),抑郁症和焦虑症。一种适合于非侵入性研究这些转运蛋白的临床方法是利用标记有短期正电子发射放射性核素的放射性药物(示踪剂)进行正电子发射断层扫描(PET)。本研究的目的是在大鼠中评估两种新型放射性示踪剂,[F] beta -CFT-FP和FFMe-McN,分别使用和方法对DAT和SERT进行成像。用众所周知的DAT示踪剂将[F] beta-CFT中的N-甲基替换为F氟丙基,显着改变了示踪剂的性能。 [F]β-CFT显示出较慢的动力学和新陈代谢,纹状体中有较高的比摄取,而[F]β-CFT-FP显示出快速的动力学和新陈代谢,纹状体中有特定的摄取。 [F] betaCFT-FP对DAT具有选择性;但是[F] beta-CFT也与去甲肾上腺素转运蛋白结合。 [F] beta-CFT-FP可能是用于对纹状体DAT部位进行成像的合适PET示踪剂,但是对于对纹状体DAT部位进行成像则需要具有更高亲和力的示踪剂。在大鼠中,FFMe-McN对SERT表现出高的靶标与非靶标比率,特异性和选择性,但动力学较慢。但是,FFMe-McN至少在临床前研究中显示出对SERT成像的潜力。此外,在PD动物模型中比较了[F]βCFT和[F] FDOPA(DA的前体)对检测轻度黑质纹状体功能低下的敏感性。 [F] FDOPA的吸收受到多巴胺能细胞补偿作用的显着影响,而[F]β-CFT更敏感,因此更适合于轻度多巴胺能症状的PET研究。总之,两种新型示踪剂[F]- CFT-FP和FFMe-McN具有潜力,但分别不是大鼠DAT和SERT成像的最佳PET示踪剂。 [F] beta-CFT优于[18F] FDOPA,可对大鼠大脑中的轻度黑色病变进行成像。

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    Marjamäki Päivi;

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  • 年度 2010
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