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使用功能性(13)N-氨正电子发射断层扫描(PET)对肝性脑病(HE)患者脑氨摄取的新发现。

New findings on cerebral ammonia uptake in HE using functional (13)N-ammonia PET.

作者信息

Sørensen Michael, Keiding Susanne

机构信息

Department of Medicine V (Hepatology), Aarhus University Hospital, Aarhus, Denmark.

出版信息

Metab Brain Dis. 2007 Dec;22(3-4):277-84. doi: 10.1007/s11011-007-9066-1.

DOI:10.1007/s11011-007-9066-1
PMID:17828586
Abstract

PET is a functional imaging technique suitable for studies of brain ammonia metabolism. Dynamic (13)N-ammonia PET yields time-courses of radioactivity concentrations in brain (PET camera) and blood (samples). Ahl et al. (Hepatology 40:73-79, 2004) and Keiding et al. (Hepatology 43:42-50, 2006) analysed such data in patients with HE by a kinetic model accounting for transfer of (13)N-ammonia across the blood-brain barrier (BBB) and intracellular formation of (13)N-glutamine. Initial unidirectional (13)N-ammonia transfer across BBB was characterized by the permeability-surface area product PS(BBB) (ml blood min(-1) ml(-1) tissue). There was a tendency to lower PS(BBB) values in patients with cirrhosis and HE than in patients with cirrhosis without HE and healthy controls but the differences were not statistically significant. Keiding et al. (Hepatology 43:42-50, 2006) also calculated PS(met) (ml blood min(-1) ml(-1) tissue) as a measure of the combined transfer of (13)N-ammonia across BBB and subsequent intracellular metabolism of (13)N-ammonia; neither did this PS-value show significant difference between the groups of subjects. Net flux of ammonia from blood into intracellular metabolites was linearly correlated to arterial ammonia. In conclusion, basic brain ammonia kinetics was not changed significantly in patients with cirrhosis +/- HE compared to healthy controls. Blood ammonia seems to be the more important factor for increased brain ammonia uptake in HE.

摘要

正电子发射断层扫描(PET)是一种适用于研究脑氨代谢的功能成像技术。动态(13)N-氨PET可得出脑(PET相机)和血液(样本)中放射性浓度随时间的变化过程。阿尔等人(《肝脏病学》40:73 - 79,2004年)和凯丁等人(《肝脏病学》43:42 - 50,2006年)通过一个动力学模型分析了肝性脑病(HE)患者的此类数据,该模型考虑了(13)N-氨穿过血脑屏障(BBB)的转运以及(13)N-谷氨酰胺的细胞内形成。最初(13)N-氨穿过BBB的单向转运以通透表面积乘积PS(BBB)(毫升血液每分钟(-1)毫升(-1)组织)为特征。肝硬化合并HE的患者与无HE的肝硬化患者及健康对照相比,PS(BBB)值有降低的趋势,但差异无统计学意义。凯丁等人(《肝脏病学》43:42 - 50,2006年)还计算了PS(met)(毫升血液每分钟(-1)毫升(-1)组织),作为(13)N-氨穿过BBB的联合转运以及随后(13)N-氨细胞内代谢的指标;该PS值在各受试者组之间也未显示出显著差异。氨从血液进入细胞内代谢物的净通量与动脉血氨呈线性相关。总之,与健康对照相比,肝硬化±HE患者的基本脑氨动力学无显著变化。血氨似乎是肝性脑病中脑氨摄取增加的更重要因素。

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