4.7 Article

Total-Body PET Multiparametric Imaging of Cancer Using a Voxelwise Strategy of Compartmental Modeling

Journal

JOURNAL OF NUCLEAR MEDICINE
Volume 63, Issue 8, Pages 1274-1281

Publisher

SOC NUCLEAR MEDICINE INC
DOI: 10.2967/jnumed.121.262668

Keywords

image processing; PET; radiotracer tissue kinetics; compartmental modeling; parametric imaging; total-body dynamic PET

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Quantitative dynamic PET with compartmental modeling allows for multiparametric imaging and more accurate quantification. This study evaluates the necessity of voxelwise compartmental modeling strategies for total-body multiparametric imaging and finds that time delay correction and model selection improve the imaging results.
Quantitative dynamic PET with compartmental modeling has the potential to enable multiparametric imaging and more accurate quantification than static PET imaging. Conventional methods for parametric imaging commonly use a single kinetic model for all image voxels and neglect the heterogeneity of physiologic models, which can work well for single-organ parametric imaging but may significantly compromise total-body parametric imaging on a scanner with a long axial field of view. In this paper, we evaluate the necessity of voxelwise compartmental modeling strategies, including time delay correction (TDC) and model selection, for total-body multiparametric imaging. Methods: Ten subjects (5 patients with metastatic cancer and 5 healthy volunteers) were scanned on a total-body PET/CT system after injection of 370 MBq of F-18-FDG. Dynamic data were acquired for 60 min. Total-body parametric imaging was performed using 2 approaches. One was the conventional method that uses a single irreversible 2-tissue-compartment model with and without TDC. The second approach selects the best kinetic model from 3 candidate models for individual voxels. The differences between the 2 approaches were evaluated for parametric imaging of microkinetic parameters and the F-18-FDG net influx rate, K-i. Results: TDC had a nonnegligible effect on kinetic quantification of various organs and lesions. The effect was larger in lesions with a higher blood volume. Parametric imaging of K-i with the standard 2-tissue-compartment model introduced vascular-region artifacts, which were overcome by the voxelwise model selection strategy. Conclusion: The time delay and appropriate kinetic model vary in different organs and lesions. Modeling of the time delay of the blood input function and model selection improved total-body multiparametric imaging.

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