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Positron Emission Tomography Quantification of 11C-Harmine Binding to Monoamine Oxidase-A in the Human Brain

机译:正电子发射断层扫描量化11c -harmine与人脑中的单胺氧化酶-A结合

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摘要

This article describes the kinetic modeling of [11C]-harmine binding to monoamine oxidase A (MAO-A) binding sites in the human brain using positron emission tomography (PET). Positron emission tomography studies were performed in healthy volunteers at placebo conditions and after treatment with clinical doses of moclobemide. In either condition, a two-tissue compartment model (2CM) provided better fits to the data than a one-tissue model. Estimates of k3/k4 values from an unconstrained 2CM were highly variable. In contrast, estimates of the specifically bound radioligand distribution volume (DVB) from an unconstrained 2CM were exceptionally stable, correlated well with the known distribution of MAO-A in the brain (cerebellum frontal cortexapproximatelyputamen temporal cortexapproximatelycingulate thalamus) and thus provided reliable indices of MAO-A density. Total distribution volume (DV) values were also highly stable and not different from those estimated with the Logan approach. Fixing the DV of free and nonspecifically bound radiotracer (DVF + NS) or coupling DVF + NS between brain regions enabled more stable estimates of k3/k4 as compared with an unconstrained 2CM. Moclobemide treatment leads to a 64% to 79% MAO-A blockade across brain regions, a result that supports the specificity of [11C]-harmine binding to MAO-A. The stability and reliability of DVB values obtained from an unconstrained 2CM, together with the computational simplicity associated with this method, support the use of DVB as an appropriate outcome measure for [11C]-harmine. These results indicate the suitability of using [11C]-harmine for quantitative evaluation of MAO-A densities using PET and should enable further studies of potential MAO-A dysregulation in several psychiatric and neurologic illnesses.
机译:本文介绍了[11C] -harmine结合使用正电子发射断层扫描(PET)在人脑网站动力学模型结合单胺氧化酶A(MAO-A)。正电子发射断层扫描研究,在安慰剂条件下健康志愿者,并与临床剂量的吗氯贝胺治疗后进行。在任一情况下,双组织隔室模型(2CM)提供了更好的配合比一组织模型中的数据。从不受约束的2CM的K3 / K4值估计是高度可变的。与此相反,从不受约束的2CM特异性结合的放射性配体的分布体积(DVB)的估计是特别稳定的,与MAO-A的在大脑中的已知分布很好的相关性(小脑<额叶cortexapproximatelyputamen <颞cortexapproximatelycingulate <丘脑),并且因此提供了可靠的MAO-A密度的指数。总分布容积(DV)值也高度稳定和那些与洛根方法估计没有什么不同。固定的自由和非特异性结合的放射性示踪剂(DVF + NS)的DV或耦合DVF + NS之间与不受约束2CM相比脑区域启用K3 / K4的更稳定的估计。吗氯贝胺治疗导致跨脑区64%到79%的MAO-A封锁,结果支持[11 C]的特异性-harmine结合MAO-A。 DVB的稳定性和可靠性值从不受约束的2CM获得,与此方法相关联的计算的简单性一起,支持使用DVB的作为适当的结果测量为[11 C] -harmine。这些结果表明,在使用[11C] -harmine的使用PET MAO-A密度的定量评价的适用性,并应使潜在的MAO-A失调的进一步研究在几个精神病和神经系统疾病。

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