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Modeling of Tracer Transport Delays for Improved Quantification of Regional Pulmonary 18F-FDG Kinetics Vascular Transit Times and Perfusion

机译:示踪剂运输延迟的模型以改进定量的区域性肺18F-FDG动力学血管运输时间和灌注。

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摘要

18F-FDG-PET is increasingly used to assess pulmonary inflammatory cell activity. However, current models of pulmonary 18F-FDG kinetics do not account for delays in 18F-FDG transport between the plasma sampling site and the lungs. We developed a three-compartment model of 18F-FDG kinetics that includes a delay between the right heart and the local capillary blood pool, and used this model to estimate regional pulmonary perfusion. We acquired dynamic 18F-FDG scans in 12 mechanically ventilated sheep divided into control and lung injury groups (n=6 each). The model was fit to tracer kinetics in three isogravitational regions-of-interest to estimate regional lung transport delays and regional perfusion. 13NN bolus infusion scans were acquired during a period of apnea to measure regional perfusion using an established reference method. The delayed input function model improved description of 18F-FDG kinetics (lower Akaike Information Criterion) in 98% of studied regions. Local transport delays ranged from 2.0–13.6s, averaging 6.4±2.9s, and were highest in non-dependent regions. Estimates of regional perfusion derived from model parameters were highly correlated with perfusion measurements based on 13NN-PET (R2=0.92, p<0.001). By incorporating local vascular transports delays, this model of pulmonary 18F-FDG kinetics allows for simultaneous assessment of regional lung perfusion, transit times, and inflammation.
机译: 18 F-FDG-PET越来越多地用于评估肺炎性细胞活性。但是,当前的肺 18 F-FDG动力学模型不能解释血浆采样点与肺之间 18 F-FDG传输的延迟。我们开发了一个三室的 18 F-FDG动力学模型,其中包括右心脏和局部毛细血管血池之间的延迟,并使用该模型来估计局部肺灌注。我们对12只机械通气的绵羊进行动态 18 F-FDG扫描,分为对照组和肺损伤组(每组n = 6)。该模型适合三个感兴趣的重力区域中的示踪动力学,以估计区域肺运输延迟和区域灌注。在呼吸暂停期间,进行了 13 NN推注输注扫描,以使用既定的参考方法测量区域灌注。延迟输入函数模型在98%的研究区域中改进了 18 F-FDG动力学(较低的赤池信息准则)的描述。本地运输延误的范围为2.0-13.6s,平均为6.4±2.9s,在非依赖地区最高。基于 13 NN-PET(R 2 = 0.92,p <0.001),基于模型参数得出的局部灌注估计值与灌注测量值高度相关。通过结合局部血管运输的延迟,这种肺 18 F-FDG动力学模型可以同时评估局部肺灌注,转运时间和炎症。

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