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通过动态正电子发射断层扫描对[11C]二氢丁苯那嗪进行动力学评估:囊泡单胺转运体的测量

Kinetic evaluation of [11C]dihydrotetrabenazine by dynamic PET: measurement of vesicular monoamine transporter.

作者信息

Koeppe R A, Frey K A, Vander Borght T M, Karlamangla A, Jewett D M, Lee L C, Kilbourn M R, Kuhl D E

机构信息

Department of Internal Medicine, University of Michigan, Ann Arbor, USA.

出版信息

J Cereb Blood Flow Metab. 1996 Nov;16(6):1288-99. doi: 10.1097/00004647-199611000-00025.

Abstract

(+)-alpha-[11C]Dihydrotetrabenazine (DTBZ) binds to the vesicular monoamine transporter (VMAT2) located in presynaptic vesicles. The purpose of this work was to evaluate various model configurations for analysis of [11C]DTBZ with the aim of providing the optimal measure of monoamine vesicular transporter density obtainable from a single dynamic PET study. PET studies on seven young normal volunteer subjects, ages 20-35, were performed following i.v. injection of 666 +/- 37 MBq (18 +/- 1 mCi) of (+)-alpha-[11C]DTBZ. Dynamic acquisition consisted of a 15-frame sequence over 1 h. Analysis methods included both creation of pixel-by-pixel functional images of transport (K1) and binding (DVtot) and nonlinear least-squares analysis of volume-of-interest data. Pixel-by-pixel calculations were performed for both two-compartment weighted integral calculations and slope-intercept estimations from Logan plots. Nonlinear least-squares analysis was performed applying model configurations with both two-compartments, estimating K1 and DVtot and three compartments, estimating K1-k4. For the more complex configuration, we examined the stability of various binding-related parameters including k3 (konBmax'), k3/k4 (Bmax'/Kd), DVsp[(K1/k2)(k3/k4)], and DVtot [K1/k2(1 + k3/k4)]. The three-compartment model provided significantly improved goodness-of-fit compared to the two-compartment model, yet did not increase the uncertainty in the estimate of the DVtot. Without constraining parameters in the three-compartment model fits, DVtot was found to provide a more stable estimate of binding density than either k3, k3/k4, or DVsp. The two-compartment least-squares analysis yielded approximately 10% underestimations of the total distribution. However, this bias was found to be very consistent from region to region as well as across subjects as indicated by the correlation between two- and three-compartment DVtot estimates of 0.997. We conclude that (+)-alpha-[11C]DTBZ and PET can provide excellent measures of VMAT2 density in the human brain.

摘要

(+)-α-[¹¹C]二氢丁苯那嗪(DTBZ)与位于突触前囊泡中的囊泡单胺转运体(VMAT2)结合。本研究的目的是评估用于分析[¹¹C]DTBZ的各种模型配置,旨在从单次动态PET研究中提供可获得的单胺囊泡转运体密度的最佳测量值。对7名年龄在20至35岁之间的年轻正常志愿者进行了PET研究,静脉注射666±37 MBq(18±1 mCi)的(+)-α-[¹¹C]DTBZ后进行。动态采集包括1小时内的15帧序列。分析方法包括创建传输(K1)和结合(DVtot)的逐像素功能图像以及感兴趣体积数据的非线性最小二乘分析。对两室加权积分计算和Logan图的斜率截距估计都进行了逐像素计算。应用两室模型配置(估计K1和DVtot)和三室模型配置(估计K1-k4)进行非线性最小二乘分析。对于更复杂的配置,我们检查了各种结合相关参数的稳定性,包括k3(konBmax')、k3/k4(Bmax'/Kd)、DVsp[(K1/k2)(k3/k4)]和DVtot [K1/k2(1 + k3/k4)]。与两室模型相比,三室模型提供了显著更好的拟合优度,但并未增加DVtot估计值的不确定性。在三室模型拟合中不限制参数的情况下,发现DVtot比k3、k3/k4或DVsp提供更稳定的结合密度估计。两室最小二乘分析得出总分布低估约10%。然而,如两室和三室DVtot估计值之间的相关性为0.997所示,发现这种偏差在不同区域以及不同受试者之间非常一致。我们得出结论,(+)-α-[¹¹C]DTBZ和PET可以提供人脑中VMAT2密度的出色测量值。

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