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Original Articles

Parameter estimation for whole-body kinetic model of FDG metabolism

, , &
Pages 1164-1170 | Received 13 Jan 2006, Published online: 17 Feb 2007
 

Abstract

Based on the radioactive tracer [18F] 2-fluoro-2-deoxy-D-gluose (FDG), positron emission tomography (PET), and compartment model, the tracer kinetic study has become an importment method to investigate the glucose metabolic kinetics in human body. In this work, the kinetic parameters of three-compartment and four-parameter model for the FDG metabolism in the tissues of myocardium, lung, liver, stomach, spleen, pancreas, and marrow were estimated through some dynamic FDG-PET experiments. Together with published brain and skeletal muscle parameters, a relatively complete whole-body model was presented. In the liver model, the dual blood supply from the hepatic artery and the portal vein to the liver was considered for parameter estimation, and the more accurate results were obtained using the dual-input rather than the single arterial-input. The established whole-body model provides the functional information of FDG metabolism in human body. It can be used to further investigate the glucose metabolism, and also be used for the simulation and visualization of FDG metabolic process in human body.

* Supported by National Natural Science Foundation of China (Grant No. 60331010)

Notes

* Supported by National Natural Science Foundation of China (Grant No. 60331010)

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