Extension: PkModeling
Acknowledgments: This work is part of the National Alliance for Medical Image Computing (NAMIC), funded by the National Institutes of Health through the NIH Roadmap for Medical Research.
Implementation of the pharmacokinetics modeling was contributed by Yingxuan Zhu and Jim Miller from GE Research.
Author: Yingxuan Zhu, Jim Miller (GE)
Contact: Yingxuan Zhu, <email>zhuyi@ge.com</email>

PkModeling (Pharmacokinetics Modeling) is to calculate the quantitative parameters from DCE-MRI images. The two major parts of it are:

• Convert signal intensities to concentration values

This is to conver signal intensities to concentration values. The concentration values will be used to calcualte quantitattive parameters next.

• Calculate quantitative parameters from concentration values. These parameters include:

Ktrans: volume transfer constant between blood plasma and EES (extracellular-extravascular space) Ve: fractional volume for extracellular space MaxSlope: maximum slope in the time series curve of one voxel AUC: area under the curve, from bolus arrival time to the end time of interval, normalized by AUC of AIF

• IO
  • Input: 4D DCE-MRI data in nrrd; 3D mask in nrrd, showing the location of arterial input function.
  • Output: 4 volumes in nrrd, showing the maps of quantitative parameters. These parameters are ktrans, ve, maximum slope, and area under the curve (AUC).
• Parameters
  • PkModeling:
    • • T1 Blood Value
      • T1 Tissue Value
      • Relaxivity Value
      • Hematocrit Value
      • AUC Time Interval Value: Time interval for AUC calculation
  • Acquisition:
    • TR Value: Repetition time,
    • TE Value: Echo time,
    • FA Value: Flip angle,
    • Time Axis: Time series.