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人体内氟-18-6-氟-L-多巴的建模。

Modeling of fluorine-18-6-fluoro-L-Dopa in humans.

作者信息

Wahl L, Nahmias C

机构信息

Department of Nuclear Medicine, McMaster University Medical Centre Hamilton, Ontario, Canada.

出版信息

J Nucl Med. 1996 Mar;37(3):432-7.

PMID:8772639
Abstract

UNLABELLED

Fluorine-18-6-fluoro-L-Dopa (F-Dopa) has been used successfully to evaluate striatal dopaminergic function in humans. The kinetic analysis of F-Dopa studies, however, is confounded by the presence of [18F]6-fluoro-3-O-methyl-L-Dopa (OMFD), the major metabolite of F-Dopa formed in the periphery that crosses the blood-brain barrier. We present results of compartmental analysis in subjects in whom we independently measured the kinetics of OMFD in the blood and striatum, and used this knowledge to solve for the kinetics of F-Dopa.

METHODS

The kinetics of F-Dopa in striatum were measured with PET from 0 to 150 min after an intravenous bolus injection of tracer in four normal subjects and two patients suffering from Parkinson's disease. On a separate occasion, the kinetics of OMFD were determined in the plasma and striatum of the same individuals. The measured OMFD kinetics of each individual allowed us to reduce the number of compartments and rate constants which have to be solved for any compartmental analysis of the kinetics of F-Dopa.

RESULTS

A two-compartmental, three rate-constant model was sufficient to describe the time course of F-Dopa and its metabolites in the striatum. The rate constant (k21) representing the decarboxylation rate of F-Dopa was 0.0124 min-1 in the normal subjects, and 0.0043 min-1 in the parkinsonian patients.

CONCLUSION

The data do not support the need to include a fourth rate constant representing the egress of F-Dopamine and its metabolites. The forward transport rates for F-Dopa and OMFD from plasma to striatum are very similar in humans.

摘要

未标注

氟-18-6-氟-L-多巴(F-Dopa)已成功用于评估人类纹状体多巴胺能功能。然而,F-Dopa研究的动力学分析因[18F]6-氟-3-O-甲基-L-多巴(OMFD)的存在而变得复杂,OMFD是F-Dopa在外周形成的主要代谢产物,可穿过血脑屏障。我们展示了在受试者中进行房室分析的结果,在这些受试者中,我们独立测量了血液和纹状体中OMFD的动力学,并利用这些知识求解F-Dopa的动力学。

方法

在4名正常受试者和2名帕金森病患者静脉推注示踪剂后0至150分钟,用PET测量纹状体中F-Dopa的动力学。在另一个时间点,测定同一受试者血浆和纹状体中OMFD的动力学。每个个体测得的OMFD动力学使我们能够减少在对F-Dopa动力学进行任何房室分析时必须求解的房室数量和速率常数。

结果

一个两房室、三个速率常数的模型足以描述纹状体中F-Dopa及其代谢产物的时间进程。代表F-Dopa脱羧速率的速率常数(k21)在正常受试者中为0.0124 min-1,在帕金森病患者中为0.0043 min-1。

结论

数据不支持需要纳入代表F-多巴胺及其代谢产物流出的第四个速率常数。在人类中,F-Dopa和OMFD从血浆到纹状体的正向转运速率非常相似。

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