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用于正电子发射断层扫描评估人脑血清素合成的[11C]-5-羟基-L-色氨酸的动力学房室模型

Kinetic compartment modeling of [11C]-5-hydroxy-L-tryptophan for positron emission tomography assessment of serotonin synthesis in human brain.

作者信息

Hagberg Gisela E, Torstenson Richard, Marteinsdottir Ina, Fredrikson Mats, Långström Bengt, Blomqvist Gunnar

机构信息

Uppsala University PET center, Institute of Psychiatry, Sweden.

出版信息

J Cereb Blood Flow Metab. 2002 Nov;22(11):1352-66. doi: 10.1097/01.WCB.0000040946.89393.9d.

Abstract

The substrate for the second enzymatic step in serotonin synthesis, 5-hydroxy-L-tryptophan, labeled in the beta-position ([11C]-HTP), was used for positron emission tomography (PET) measurements in six healthy human participants, examined on two occasions. One- and two-tissue kinetic compartment modeling of time-radioactivity curves was performed, using arterial, metabolite-corrected [11C]-HTP values as input function. The availability of unchanged tracer in arterial blood plasma was > or = 80% up to 60 minutes after injection, while [11C]-hydroxyindole acetic acid and [11C]-serotonin accounted for the remaining radioactivity, amounting to < or = 16% and < or = 4%, respectively. Compartment modeling was performed for brain stem, putamen, caudate nucleus, anterior cingulate, white matter, and superior occipital, occipitotemporal, and temporal cortices. The average biologic half-life for plasma-to-tissue equilibrium was 7 to 12 minutes, and the volume of distribution was 0.2 to 0.5 microL.mL(-1). In all regions except white matter, the kinetic compartment model that included irreversible [11C]-HTP trapping showed significantly improved model fits with respect to a one-tissue compartment model. The [11C]-HTP trapping rate constant depended on the estimated tissue availability of the serotonin precursor tryptophan, known to reflect serotonin synthesis in healthy individuals, and correlated with serotonin tissue concentration and synthesis rates reported previously in literature. These findings suggest the use of [11C]-HTP PET measurements to investigate serotonin synthesis.

摘要

血清素合成第二步酶促反应的底物5-羟基-L-色氨酸在β位标记([11C]-HTP),用于对6名健康人类受试者进行正电子发射断层扫描(PET)测量,分两次进行检查。使用动脉血中代谢物校正后的[11C]-HTP值作为输入函数,对时间-放射性曲线进行单组织和双组织动力学房室模型分析。注射后60分钟内,动脉血浆中未变化的示踪剂可用性≥80%,而[11C]-羟基吲哚乙酸和[11C]-血清素分别占其余放射性的≤16%和≤4%。对脑干、壳核、尾状核、前扣带回、白质以及枕叶上部、枕颞叶和颞叶皮质进行了房室模型分析。血浆与组织达到平衡的平均生物半衰期为7至12分钟,分布容积为0.2至0.5 μL·mL-1。在除白质外的所有区域,包含不可逆[11C]-HTP捕获的动力学房室模型相对于单组织房室模型显示出显著改善的模型拟合。[11C]-HTP捕获速率常数取决于血清素前体色氨酸的估计组织可用性,已知其反映健康个体中的血清素合成,并且与先前文献报道的血清素组织浓度和合成速率相关。这些发现表明可使用[11C]-HTP PET测量来研究血清素合成。

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