评估人脑中的[11C]UCB-A 正电子发射断层扫描。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Mengfei Xiong, Mark Lubberink, Lieuwe Appel, Xiaotian Tsong Fang, Torsten Danfors, Eva Kumlien, Gunnar Antoni
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引用次数: 0

摘要

背景:在临床前研究中,[11C]UCB-A 正电子发射断层扫描(PET)成像为突触囊泡蛋白 2A (SV2A)作为突触密度的替代物提供了很好的成像结果。本文报告了首次人体[11C]UCB-A PET研究,以确定其在健康受试者体内的动力学特征,并进一步评估 SV2A 的特异性结合:12名健康受试者接受了90分钟的PET/MRI[11C]UCB-A基线扫描,其中两名受试者在服用单剂量左乙拉西坦(1500毫克)后参加了额外的阻断扫描,扫描过程相同。我们的研究结果表明,大脑皮层所有区域都摄取了大量的[11C]UCB-A,且消除速度较慢。使用各种区室模型对[11C]UCB-A PET进行动力学建模表明,不可逆的双组织区室模型最能描述放射性示踪剂的动力学。因此,采用 Patlak 图形分析法来简化分析。拉森图确定的 SV2A 占位率估计约为 66%。基线时的特异性结合和与灰质相当的结合减少排除了将半叶中心作为参考组织的可能性:结论:[11C]UCB-A PET 成像可量化体内 SV2A。结论:[11C]UCB-A PET 成像可量化体内 SV2A,但其缓慢的动力学要求较长的扫描时间,而碳-11 的半衰期较短,这是不现实的。因此,缓慢的动力学和复杂的量化方法可能会限制其在人体中的应用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Evaluation of [11C]UCB-A positron emission tomography in human brains.

Background: In preclinical studies, the positron emission tomography (PET) imaging with [11C]UCB-A provided promising results for imaging synaptic vesicle protein 2A (SV2A) as a proxy for synaptic density. This paper reports the first-in-human [11C]UCB-A PET study to characterise its kinetics in healthy subjects and further evaluate SV2A-specific binding.

Results: Twelve healthy subjects underwent 90-min baseline [11C]UCB-A scans with PET/MRI, with two subjects participating in an additional blocking scan with the same scanning procedure after a single dose of levetiracetam (1500 mg). Our results indicated abundant [11C]UCB-A brain uptake across all cortical regions, with slow elimination. Kinetic modelling of [11C]UCB-A PET using various compartment models suggested that the irreversible two-tissue compartment model best describes the kinetics of the radioactive tracer. Accordingly, the Patlak graphical analysis was used to simplify the analysis. The estimated SV2A occupancy determined by the Lassen plot was around 66%. Significant specific binding at baseline and comparable binding reduction as grey matter precludes the use of centrum semiovale as reference tissue.

Conclusions: [11C]UCB-A PET imaging enables quantifying SV2A in vivo. However, its slow kinetics require a long scan duration, which is impractical with the short half-life of carbon-11. Consequently, the slow kinetics and complicated quantification methods may restrict its use in humans.

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CiteScore
7.20
自引率
4.30%
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