Pharmacokinetic modeling of DCE-MRI is based on fitting perfusion parameters to contrast agent concentration or relaxivity curves computed using the nonlinear spoiled gradient-echo (SPGR) signal equation, T1 mapping values, and the linear relationship between T1 and contrast agent relaxivity. The nonlinear term of the SPGR equation has implications for how image noise scales in the concentration. By simulating image noise at different levels for ideal curves of different parameter values, we show why it’s advantageous to fit signal intensity curves rather than relaxivity curves.
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