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首页> 外文期刊>Journal of Cerebral Blood Flow and Metabolism: Official Journal of the International Society of Cerebral Blood Flow and Metabolism >Dual time-point imaging for post-dose binding potential estimation applied to a [C-11]raclopride PET dose occupancy study
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Dual time-point imaging for post-dose binding potential estimation applied to a [C-11]raclopride PET dose occupancy study

机译:用于后剂量结合潜在估计的双时间点成像应用于[C-11] raclopride PET剂量占用研究

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Receptor occupancy studies performed with PET often require time-consuming dynamic imaging for baseline and post-dose scans. Shorter protocol approximations based on standard uptake value ratios have been proposed. However, such methods depend on the time-point chosen for the quantification and often lead to overestimation and bias. The aim of this study was to develop a shorter protocol for the quantification of post-dose scans using a dual time-point approximation, which employs kinetic parameters from the baseline scan. Dual time-point was evaluated for a [C-11]raclopride PET dose occupancy study with the D2 antagonist JNJ-37822681, obtaining estimates for binding potential and receptor occupancy. Results were compared to standard simplified reference tissue model and standard uptake value ratios-based estimates. Linear regression and Bland-Altman analysis demonstrated excellent correlation and agreement between dual time-point and the standard simplified reference tissue model approach. Moreover, the stability of dual time-point-based estimates is shown to be independent of the time-point chosen for quantification. Therefore, a dual time-point imaging protocol can be applied to post-dose [C-11]raclopride PET scans, resulting in a significant reduction in total acquisition time while maintaining accuracy in the quantification of both the binding potential and the receptor occupancy.
机译:用宠物进行的受体占用研究经常需要耗时的动态成像,用于基线和后剂量扫描。已经提出了基于标准摄取值比的较短协议近似。然而,这些方法取决于为量化选择的时间点,并且通常导致高估和偏置。本研究的目的是使用双时间点近似来制定较短的较短协议,用于使用从基线扫描中采用动力学参数的双时间点近似进行剂量扫描。评估双时间点的液相点,用于用D2拮抗剂JNJ-37822681评价[C-11] raclopride PET剂量占用性研究,获得结合潜力和受体占用的估计。将结果与标准简化的参考组织模型和标准摄取价值比率进行比较。线性回归和Bland-Altman分析显示了双重时间点与标准简化参考组织模型方法的出色相关性和协议。此外,基于双时间点的估计的稳定性被证明与所选择的定量点无关。因此,可以将双重时间点成像协议应用于剂量后[C-11] Raclopride PET扫描,导致总获取时间显着降低,同时保持粘合潜力和受体占用的定量精度。

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