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N-[11C-甲基]氯苯丁胺和N,N-[11C-二甲基]氯苯丁胺作为正电子发射断层扫描的脑血流显像剂

N-[11C-Methyl]chlorphentermine and N,N-[11C-dimethyl]chlorphentermine as brain blood-flow agents for positron emission tomography.

作者信息

Kizuka H, Elmaleh D R, Boudreaux G J, Strauss H W, Ackerman R H, Brownell G L

出版信息

J Nucl Med. 1986 Apr;27(4):532-7.

PMID:3486957
Abstract

N-[11C-methyl]chlorphentermine ([11C]NMCP) and N,N-[11C-dimethyl]chlorphentermine ([11C]NDMCP) were prepared from chlorphentermine and 11CH3I in DMF and evaluated in rats as brain blood-flow agents for positron emission tomography (PET). Tissue distribution of [11C]NMCP showed that brain uptake was 2.70 +/- 0.40% of injected dose per organ at 5 min with no change in radioactivity concentration up to 30 min after i.v. injection. Approximately 80% of the initial brain uptake remained at 60 min. On the other hand, initial brain uptake of [11C] NDMCP (3.66 +/- 0.31 and 3.63 +/- 0.88% injected dose per organ at 5 and 15 min, respectively) was greater than that of [11C]NMCP. The brain activity however, rapidly decreased to 2.38 +/- 0.17 and 1.82 +/- 0.32% at 30 and 60 min, respectively. Because of its longer retention in the brain compared with [11C]NDMCP, [11C]NMCP would be a potential brain blood-flow agent for quantitative PET studies.

摘要

N-[11C-甲基]氯苯丙胺([11C]NMCP)和N,N-[11C-二甲基]氯苯丙胺([11C]NDMCP)由氯苯丙胺和11CH3I在N,N-二甲基甲酰胺中制备,并在大鼠中作为正电子发射断层扫描(PET)的脑血流显像剂进行评估。[11C]NMCP的组织分布显示,静脉注射后5分钟时脑摄取量为每器官注射剂量的2.70±0.40%,直至30分钟放射性浓度无变化。静脉注射后60分钟时,约80%的初始脑摄取量仍保留。另一方面,[11C]NDMCP的初始脑摄取量(分别在5分钟和15分钟时为每器官注射剂量的3.66±0.31%和3.63±0.88%)高于[11C]NMCP。然而,脑放射性活度在30分钟和60分钟时分别迅速降至2.38±0.17%和1.82±0.32%。由于与[11C]NDMCP相比,[11C]NMCP在脑中的滞留时间更长,因此它可能是用于PET定量研究的脑血流显像剂。

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