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无酪氨酸氨基酸混合物减轻苯丙胺诱导的[11C]雷氯必利在体内纹状体中的置换:一项大鼠PET研究。

Tyrosine-free amino acid mixture attenuates amphetamine-induced displacement of [11C]raclopride in striatum in vivo: a rat PET study.

作者信息

Le Masurier Marisa, Houston Gavin, Cowen Philip, Grasby Paul, Sharp Trevor, Hume Susan

机构信息

University Department of Pharmacology, Mansfield Road, Oxford OX1 3QT, UK.

出版信息

Synapse. 2004 Feb;51(2):151-7. doi: 10.1002/syn.10285.

Abstract

Previous neurochemical and behavioural studies show that tyrosine depletion using a nutritionally balanced tyrosine-free amino acid mixture attenuates the dopamine-releasing and psychostimulant properties of amphetamine. Here we investigate the effect of a tyrosine-free amino acid mixture on striatal binding of [(11)C]raclopride, and amphetamine-induced [(11)C]raclopride displacement, using positron emission tomography in the rat. Rats were scanned for 60 min after an i.v. injection of approximately 11 MBq [(11)C]raclopride using a quad-HIDAC system. Amphetamine (2 mg/kg i.p., 30 min prior to scan) caused a 12% reduction in [(11)C]raclopride distribution volume ratio (DVR) compared to saline-injected controls. The tyrosine-free amino acid mixture (1 g/kg i.p.) caused a small (+7%) but statistically insignificant increase in [(11)C]raclopride DVR and attenuated, although it did not fully block, the amphetamine-induced reduction. These data are in keeping with previous neurochemical, immunocytochemical, and behavioural studies showing that tyrosine-free amino acid mixtures reduce dopamine function and offer promise for future PET studies testing the effect of tyrosine-depleting paradigms on dopamine release in humans.

摘要

先前的神经化学和行为学研究表明,使用营养均衡的无酪氨酸氨基酸混合物使酪氨酸耗竭,可减弱苯丙胺的多巴胺释放和精神刺激特性。在此,我们利用正电子发射断层扫描技术,研究了无酪氨酸氨基酸混合物对大鼠纹状体中[(11)C]雷氯必利结合以及苯丙胺诱导的[(11)C]雷氯必利取代的影响。使用四探头HIDAC系统,在静脉注射约11 MBq [(11)C]雷氯必利后,对大鼠进行60分钟的扫描。与注射生理盐水的对照组相比,苯丙胺(腹腔注射2 mg/kg,扫描前30分钟)使[(11)C]雷氯必利分布体积比(DVR)降低了12%。无酪氨酸氨基酸混合物(腹腔注射1 g/kg)使[(11)C]雷氯必利DVR有小幅升高(+7%),但无统计学意义,并且尽管未完全阻断,但减弱了苯丙胺诱导的降低。这些数据与先前的神经化学、免疫细胞化学和行为学研究一致,表明无酪氨酸氨基酸混合物可降低多巴胺功能,并为未来测试酪氨酸耗竭模式对人类多巴胺释放影响的PET研究提供了前景。

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