Michael Germuska1, Sophie Riches1,
David Collins1, Geoffrey Payne1, Nandita deSouza1,
Martin Leach1, Matthew Orton1
1CR-UK and EPSRC Cancer Imaging Centre,
Institute of Cancer Research and
Dynamic
contrast enhanced MRI requires an estimate or measurement of the arterial
input function (AIF) to model pharmacokinetic behaviour. To reduce the
variability in a measured AIF, a population AIF is often used. Alternatively
it is possible to obtain an AIF from local tissue. Pharmacokinetic models
driven by AIFs extracted from the prostate tissue were compared to a
population AIF for 12 prostate cancer patients. Tissue estimated AIFs were
found to out performed the population AIF in terms of fitting residuals and
variability in KTrans estimates. The results show tissue estimated AIFs can
be used to improve DCE-MRI model fitting.