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在晚期帕金森病中,用正电子发射断层扫描(PET)研究恩他卡朋抑制儿茶酚-O-甲基转移酶(COMT)后纹状体[18F]氟多巴的利用情况。

Striatal [18F]fluorodopa utilization after COMT inhibition with entacapone studied with PET in advanced Parkinson's disease.

作者信息

Ruottinen H M, Rinne J O, Ruotsalainen U H, Bergman J R, Oikonen V J, Haaparanta M T, Solin O H, Laihinen A O, Rinne U K

机构信息

Department of Neurology, University of Turku, Finland.

出版信息

J Neural Transm Park Dis Dement Sect. 1995;10(2-3):91-106. doi: 10.1007/BF02251225.

Abstract

The effect of peripheral catechol-O-methyltransferase (COMT) inhibition with entacapone on striatal uptake of 6-[18F]fluoro-L-dopa (FDOPA) was studied with PET both without and with entacapone in fifteen advanced parkinsonian patients and six healthy controls. Entacapone significantly enhanced the fraction of unmetabolized FDOPA in plasma from 16% to about 50% at 80 minutes after FDOPA injection in all subjects. The striatal to occipital ratios and the striatal FDOPA uptake, expressed as a modified decarboxylation coefficient (k3R0), was significantly increased in healthy controls, whereas in parkinsonian patients the increase was significant only in the caudate. On the other hand, the influx constant (Ki) decreased significantly in the caudate and putamen in parkinsonian patients; in healthy controls the Ki remained virtually unchanged. Effective peripheral COMT inhibition markedly increased the fraction of FDOPA in plasma and thus its availability in the brain for decarboxylation both in patients and control subjects. However, the change in striatal FDOPA uptake was modest in the advanced parkinsonian patients as compared to that in control subjects, because of the advanced disease, decreased storage capacity, or both.

摘要

在15例晚期帕金森病患者和6名健康对照者中,采用正电子发射断层扫描(PET)研究了恩他卡朋抑制外周儿茶酚-O-甲基转移酶(COMT)对纹状体摄取6-[18F]氟-L-多巴(FDOPA)的影响,研究分为未使用恩他卡朋和使用恩他卡朋两种情况。在所有受试者中,恩他卡朋显著提高了FDOPA注射后80分钟时血浆中未代谢FDOPA的比例,从16%提高到约50%。健康对照者的纹状体与枕叶比值以及以修正脱羧系数(k3R0)表示的纹状体FDOPA摄取量显著增加,而在帕金森病患者中,仅尾状核的增加具有显著性。另一方面,帕金森病患者尾状核和壳核的流入常数(Ki)显著降低;在健康对照者中,Ki基本保持不变。有效的外周COMT抑制显著增加了血浆中FDOPA的比例,从而增加了其在患者和对照者大脑中用于脱羧的可用性。然而,与对照者相比,晚期帕金森病患者纹状体FDOPA摄取的变化较小,这是由于疾病晚期、储存能力下降或两者兼而有之。

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