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Improved models for plasma radiometabolite correction and their impact on kinetic quantification in PET studies

机译:改进的血浆放射性代谢物校正模型及其对PET研究中动力学定量的影响

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摘要

The quantification of dynamic positron emission tomography studies performed with arterial sampling usually requires correcting the input function for the presence of radiometabolites by using a model of the plasma parent fraction (PPf). Here, we show how to include the duration of radioligand injection in the PPf model formulations to achieve a more physiologic description of the plasma measurements. This formulation (here called convoluted model) was tested on simulated data and on three datasets with different parent kinetics: [11C]NOP-1A, [11C]MePPEP, and [11C](R)-rolipram. Results showed that convoluted PPf models better described the fraction of unchanged parent in the plasma compared with standard models for all three datasets (weighted residuals sum of squares up to 25% lower). When considering the effect on tissue quantification, the overall impact on the total volume of distribution (VT) was low. However, the impact was significant and radioligand-dependent on the binding potential (BP) and the microparameters (K1, k2, k3, and k4). Simulated data confirmed that quantification is sensitive to different degrees to PPf model misspecification. Including the injection duration allows obtaining a more accurate correction of the input function for the presence of radiometabolites and this yields a more reliable quantification of the tissue parameters.
机译:用动脉采样进行的动态正电子发射断层扫描研究的量化通常需要通过使用血浆母体组分(PPf)模型校正放射性代谢物存在的输入函数。在这里,我们展示了如何在PPf模型配方中包括放射性配体注射的持续时间,以实现血浆测量的更生理描述。在模拟数据和具有不同母体动力学的三个数据集上测试了此公式(这里称为卷积模型):[ 11 C] NOP-1A,[ 11 C] MePPEP,和[ 11 C](R)-咯利普兰。结果表明,与所有三个数据集的标准模型相比,卷积的PPf模型更好地描述了血浆中未改变的亲本的比例(加权残差平方和降低了25%)。考虑对组织定量的影响时,对总分布体积(VT)的总体影响很小。但是,这种影响是巨大的,并且放射性配体取决于结合电位(BP)和微参数(K1,k2,k3和k4)。模拟数据证实,量化对PPf模型错误指定在不同程度上敏感。包括注射时间在内,可以对放射性代谢物的存在获得更准确的输入函数校正,从而产生对组织参数更可靠的量化。

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