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[(18)F]阿坦色林静脉推注PET数据的分析。II:人体中放射性标记代谢物的考量。

Analyses of [(18)F]altanserin bolus injection PET data. II: consideration of radiolabeled metabolites in humans.

作者信息

Price J C, Lopresti B J, Meltzer C C, Smith G S, Mason N S, Huang Y, Holt D P, Gunn R N, Mathis C A

机构信息

Department of Radiology, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania 15213, USA.

出版信息

Synapse. 2001 Jul;41(1):11-21. doi: 10.1002/syn.1055.

Abstract

Imaging serotonin-2A (5-HT(2A)) neuroreceptors with positron emission tomography (PET) and [(18)F]altanserin has been the focus of a series of PET studies, as [(18)F]altanserin is one of the most selective 5-HT(2A) antagonist radiotracers. Previous animal studies showed that radiolabeled metabolites (radiometabolites) of [(18)F]altanserin crossed the blood-brain barrier (BBB) to localize nonspecifically in brain, consistent with a constant radioactivity "background." In this work, we evaluated human bolus injection [(18)F]altanserin PET data with detailed consideration of the impact of BBB-permeable metabolites on the specific binding parameters. Data were quantified using either single (parent radiotracer), dual (parent radiotracer and radiometabolites), or no arterial input function(s) (cerebellum as reference tissue input function). A step-gradient high-performance liquid chromatography (HPLC) analysis provided distinct separation of [(18)F]altanserin and four radiolabeled components in plasma. After [(18)F]altanserin injection, the step-gradient data showed that the major BBB-permeable radiometabolites approached constant levels in plasma (>50 min), consistent with a constant metabolite "background." The single-input Logan graphical results were highly correlated with the dual-input results and its bias was fairly constant across regions and subjects, as similarly observed for a nongraphical reference tissue method. The most comprehensive and quantitatively valid analysis for bolus [(18)F]altanserin PET data was the dual-input method that specifically accounted for BBB-permeable metabolites, although the Logan analysis was preferred because it provided a good compromise between validity, sensitivity, and reliability of implementation. Further study is needed to better understand how the cerebellar kinetics of [(18)F]altanserin and its radiometabolites impact the reference tissue measures.

摘要

用正电子发射断层扫描(PET)和[¹⁸F]阿坦色林对5-羟色胺-2A(5-HT₂A)神经受体进行成像一直是一系列PET研究的重点,因为[¹⁸F]阿坦色林是最具选择性的5-HT₂A拮抗剂放射性示踪剂之一。先前的动物研究表明,[¹⁸F]阿坦色林的放射性标记代谢物(放射性代谢物)穿过血脑屏障(BBB),在脑中非特异性定位,这与恒定的放射性“本底”一致。在这项工作中,我们在详细考虑BBB可渗透代谢物对特异性结合参数影响的情况下,评估了人体静脉注射[¹⁸F]阿坦色林PET数据。使用单一(母体放射性示踪剂)、双重(母体放射性示踪剂和放射性代谢物)或无动脉输入函数(小脑作为参考组织输入函数)对数据进行定量。梯度高效液相色谱(HPLC)分析可清晰分离血浆中的[¹⁸F]阿坦色林和四种放射性标记成分。注射[¹⁸F]阿坦色林后,梯度数据显示主要的BBB可渗透放射性代谢物在血浆中达到恒定水平(>50分钟),这与恒定的代谢物“本底”一致。单输入Logan图像结果与双输入结果高度相关,并且其偏差在不同区域和受试者之间相当恒定,这与非图像参考组织方法的观察结果相似。对于静脉注射[¹⁸F]阿坦色林PET数据,最全面且定量有效的分析方法是双输入方法,该方法专门考虑了BBB可渗透代谢物,不过Logan分析更受青睐,因为它在有效性、灵敏度和实施可靠性之间提供了良好的折衷。需要进一步研究以更好地了解[¹⁸F]阿坦色林及其放射性代谢物的小脑动力学如何影响参考组织测量。

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