| Journal of Nuclear Medicine | |
| Searching for Alternatives to Full Kinetic Analysis in 18F-FDG PET: An Extension of the Simplified Kinetic Analysis Method | |
| Jorge A. Carrasquillo1 Sebastien Hapdey1 Irene Buvat1 Millie Whatley1 Joan M. Carson1 Stephen L. Bacharach1 | |
| 关键词: oncology; PET; radiotracer tissue kinetics; Patlak; simplified kinetic analysis; | |
| DOI : 10.2967/jnumed.110.079079 | |
| 学科分类:医学(综合) | |
| 来源: Society of Nuclear Medicine | |
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【 摘 要 】
The most accurate way to estimate the glucose metabolic rate (or its influx constant) from 18F-FDG PET is to perform a full kinetic analysis (or its simplified Patlak version), requiring dynamic imaging and the knowledge of arterial activity as a function of time. To avoid invasive arterial blood sampling, a simplified kinetic analysis (SKA) has been proposed, based on blood curves measured from a control group. Here, we extend the SKA by allowing for a greater variety of arterial input function (A(t)) curves among patients than in the original SKA and by accounting for unmetabolized 18F-FDG in the tumor. Methods: Ten A(t)s measured in patients were analyzed using a principal-component analysis to derive 2 principal components describing most of the variability of the A(t). The mean distribution volume of 18F-FDG in tumors for these patients was used to estimate the corresponding quantity in other patients. In subsequent patient studies, the A(t) was described as a linear combination of the 2 principal components, for which the 2 scaling factors were obtained from an early and a late venous sample drawn for the patient. The original and extended SKA (ESKA) were assessed using fifty-seven 18F-FDG PET scans with various tumor types and locations and using different injection and acquisition protocols, with the Ki derived from Patlak analysis as a reference. Results: ESKA improved the accuracy or precision of the input function (area under the blood curve) for all protocols examined. The mean errors (±SD) in Ki estimates were −12% ± 33% for SKA and −7% ± 22% for ESKA for a 20-s injection protocol with a 55-min postinjection PET scan, 20% ± 42% for SKA and 1% ± 29% for ESKA (P < 0.05) for a 120-s injection protocol with a 55-min postinjection PET scan, and −37% ± 19% for SKA and −4% ± 6% for ESKA (P < 0.05) for a 20-s injection protocol with a 120-min postinjection PET scan. Changes in Ki between the 2 PET scans in the same patients also tended to be estimated more accurately and more precisely with ESKA than with SKA. Conclusion: ESKA, compared with SKA, significantly improved the accuracy and precision of Ki estimates in 18F-FDG PET. ESKA is more robust than SKA with respect to various injection and acquisition protocols.
【 授权许可】
Unknown
【 预 览 】
| Files | Size | Format | View |
|---|---|---|---|
| RO201912010198079ZK.pdf | 758KB |  download |
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