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11C标记的左旋多巴和氟代左旋多巴作为用于突触前多巴胺能系统的正电子发射断层扫描示踪剂的比较。

A comparison of 11C-labeled L-DOPA and L-fluorodopa as positron emission tomography tracers for the presynaptic dopaminergic system.

作者信息

Torstenson R, Tedroff J, Hartvig P, Fasth K J, Långström B

机构信息

The Subfemtomole Biorecognition Project, Uppsala University and Japanese Research and Development Council, Sweden.

出版信息

J Cereb Blood Flow Metab. 1999 Oct;19(10):1142-9. doi: 10.1097/00004647-199910000-00011.

Abstract

11C-labeled 3,4-Dihydroxy-phenyl-L-alanine (L-DOPA) and L-fluorodopa were used as tracers for the functional state of the presynaptic dopamine system in anesthetized monkeys with positron emission tomography. The radiotracer disposition in brain tissue and plasma were studied and effects induced by pharmacologic challenges were evaluated. 6R-L-erythro-5,6,7,8-tetrahydrobiopterin (6R-BH4) increased the striatal influx rate constant, e.g., striatal K(i) for L-[beta-11C]DOPA, but it induced no effect on the K(i)-value using L-[beta-11C]-6-fluorodopa. Studies of radiolabeled tracer and metabolites in plasma showed substantial differences between the two tracers. At baseline conditions, 60% unchanged L-[beta-11C]DOPA was detected in plasma 50 minutes after tracer injection and the 3-O-methylated fraction accounted for 25% of total radioactivity. For L-[beta-11C]-6-fluorodopa, the relation was inverse; about 25% unchanged tracer and 60% 3-O-methyl metabolite were present in plasma after 50 minutes. A site-specific 11C-labeling in the carboxylic position in the molecules revealed a significant specific retention of radioactivity in striatum with L-[car-boxy-11C]-6-fluorodopa but not with L-[carboxy-11C]DOPA. The 3-O-methyl metabolite of L-DOPA is known to pass the blood-brain barrier and may interfere with the calculation of the K(i)value using a brain reference region. Thus, extensive 3-O-methylation in circulation of the fluorinated analog could obscure the detectability of potential functional change in striatal K(i) of the tracer when using a reference tissue model for calculation.

摘要

11C标记的3,4-二羟基苯丙氨酸(L-DOPA)和L-氟多巴被用作正电子发射断层扫描麻醉猴中突触前多巴胺系统功能状态的示踪剂。研究了放射性示踪剂在脑组织和血浆中的分布,并评估了药理学激发所诱导的效应。6R-L-赤藓糖-5,6,7,8-四氢生物蝶呤(6R-BH4)增加了纹状体流入速率常数,例如L-[β-11C]多巴的纹状体K(i),但使用L-[β-11C]-6-氟多巴时对K(i)值没有影响。血浆中放射性标记示踪剂和代谢物的研究表明两种示踪剂之间存在显著差异。在基线条件下,示踪剂注射后50分钟血浆中检测到60%未变化的L-[β-11C]多巴,3-O-甲基化部分占总放射性的25%。对于L-[β-11C]-6-氟多巴,情况相反;50分钟后血浆中存在约25%未变化的示踪剂和60%的3-O-甲基代谢物。分子中羧基位置的位点特异性11C标记显示,L-[羧基-11C]-6-氟多巴在纹状体中有显著的放射性特异性保留,而L-[羧基-11C]多巴则没有。已知L-DOPA的3-O-甲基代谢物可通过血脑屏障,并可能干扰使用脑参考区域计算K(i)值。因此,当使用参考组织模型进行计算时,氟化类似物在循环中的广泛3-O-甲基化可能会掩盖示踪剂纹状体K(i)中潜在功能变化的可检测性。

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