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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 >Substitution of venous for arterial blood sampling in the determination of regional rates of cerebral protein synthesis with L-[1-C-11]leucine PET: A validation study
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Substitution of venous for arterial blood sampling in the determination of regional rates of cerebral protein synthesis with L-[1-C-11]leucine PET: A validation study

机译:动脉血样取静脉归因于L- [1-C-11]亮氨酸宠物:验证研究确定脑蛋白合成区域率

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We developed and validated a method to estimate input functions for determination of regional rates of cerebral protein synthesis (rCPS) with L-[1-C-11]leucine PET without arterial sampling. The method is based on a population-derived input function (PDIF) approach, with venous samples for calibration. Population input functions were constructed from arterial blood data measured in 25 healthy 18-24-year-old males who underwent L-[1-C-11]leucine PET scans while awake. To validate the approach, three additional groups of 18-27-year-old males underwent L-[1-C-11]leucine PET scans with both arterial and venous blood sampling: 13 awake healthy volunteers, 10 sedated healthy volunteers, and 5 sedated subjects with fragile X syndrome. Rate constants of the L-[1-C-11]leucine kinetic model were estimated voxel-wise with measured arterial input functions and with venous-calibrated PDIFs. Venous plasma leucine measurements were used with venous-calibrated PDIFs for rCPS computation. rCPS determined with PDIFs calibrated with 30-60 min venous samples had small errors (RMSE: 4-9%), and no statistically significant differences were found in any group when compared to rCPS determined with arterial input functions. We conclude that in young adult males, PDIFs calibrated with 30-60 min venous samples can be used in place of arterial input functions for determination of rCPS with L-[1-C-11]leucine PET.
机译:我们开发并验证了一种估算了在没有动脉抽样的L- [1-C-11]亮氨酸肽的脑蛋白合成(RCP)的区域率测定的输入功能的方法。该方法基于群体衍生的输入功能(PDIF)方法,具有静脉样品进行校准。人口输入功能由25例健康18-24岁男性测量的动脉血数据构成,醒来时患有L- [1-C-11]亮氨酸疫苗。为了验证这种方法,三个额外的18-27岁男性幼儿患有动脉和静脉血液取样的L-[1-C-11]亮氨酸扫描:13令人醒着的健康志愿者,10名镇静健康志愿者,5沉积物X综合征患有脆弱的主体。 L- [1-C-11]亮氨酸动力学模型的速率常数估计具有测量的动脉输入功能和静脉校准PDIFs的体素。静脉血浆亮氨酸测量与RCPS计算的静脉校准PDIF一起使用。用30-60分钟的静脉样品校准的PDIF测定的RCP具有小的误差(RMSE:4-9%),与随动脉输入函数测定的RCP相比,在任何组中没有发现统计学意义的差异。我们得出结论,在年轻的成年男性中,可以使用用30-60分钟的静脉样品进行校准的PDIFs代替动脉输入功能,以确定R-[1-C-11]亮氨酸宠物的RCP。

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