- 作者:Á ; dá ; m Vas ; Yevgeni Shchukin ; Virginija D. Karrenbauer ; Zsolt Cselé ; nyi ; Kosta Kostulas ; Jan Hillert ; Ivanka Savic ; Akihiro Takano ; Christer Halldin ; Balá ; zs Gulyá ; s
- 关键词:Vinpocetine ; PK11195 ; Peripheral benzodiazepine binding site ; Glia ; Positron emission tomography ; Sclerosis multiplex
- 刊名:Journal of the Neurological Sciences
- 出版年:2008
- 出版时间:15 January 2008
- 年:2008
- 卷:264
- 期:1-2
- 页码:9-17
- 全文大小:2770 K
However, regional BP values for [11C]vinpocetine were markedly higher than those for [11C]PK11195. This feature of the former radioligand may be related to its high brain uptake and marked affinity to the peripheral benzodiazepine receptor binding sites (PBBS), characteristic for glia cells. As local brain traumas entail reactive glia accumulation in and around the site of the damage, the present findings may indicate that [11C]vinpocetine marks the place or boundaries of local brain damage by binding to the PBBS present in glia cells, which, in turn, accumulate in the region of the damage.
The present findings (i) confirm earlier observations with [11C]PK11195 as a potential glia marker in PET studies and (ii) support the working hypothesis that [11C]vinpocetine is a potentially useful PET marker of regional and global brain damage resulting in glia accumulation locally or globally in the human brain. The comparative analysis of the two ligands indicate that [11C]vinpocetine shows a number of characteristics favourable in comparison with [11C]PK11195.