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GENERATION OF PARAMETRIC IMAGES

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Title: GENERATION OF PARAMETRIC IMAGES


1
GENERATION OF PARAMETRIC IMAGES
  • PROSPECTS
  • PROBLEMS

Vesa Oikonen Turku PET Centre 2004-03-25
2
Multiple-Time Graphical Analysis
  • Gjedde-Patlak plot for irreversible uptake
  • Logan plot for reversible uptake
  • Independent on model structure
  • Plasma and reference tissue input
  • Fast computation
  • Available everywhere

3
Multiple-Time Graphical Analysis
  1. Regional analysis to determine the time when plot
    becomes linear
  2. For Logan analysis with reference tissue input
    compartment model fit to determine population
    average of reference tissue k2

4
Multiple-Time Graphical Analysis
  • Examples of DV and DVR images

5
Multiple-Time Graphical Analysis
  • Different regions have different kinetics
  • Usually linear phase is reached later in regions
    of high uptake
  • Solution select fit range separately for each
    pixel

6
Multiple-Time Graphical Analysis
Nr of frames used in line fit(darkermore frames
DVR image where fit range was determined separatel
y for each pixel
7
Compartmental model fit
  • Also time before equilibrium is used in the fit
  • Parametersare solvedfrommultilinearequations

8
Compartmental model fit
  • Fast computation from multilinear equations with
    standard techniques
  • Multilinear equations can be transformed to solve
    macroparameters (DV or Ki) without division

9
Compartmental model fit
DV
10
Compartmental model fit
  • Pixel-by-pixel selection between 2CM and 3CM
    based on Akaike Information Criteria (AIC), or
  • Akaike weighted average of DV from 2CM and 3CM
    fits (Turkheimer et al 2003)

11
Compartmental model fit
Relative weights of2CM (white) and 3CM
(black)based on AIC
Akaike weighted average ofDV from 2CM and 3CM
12
Compartmental model fit
  • Alternative to Akaike weightingLawson-Hanson
    non-negative least-squares (NNLS) produces
    good-quality DV and DVR images from multilinear
    3CM

13
Simplified Reference Tissue Method (SRTM)
Binding Potential (BP) solved using
  • Basis Function Method (BFM)
  • Multilinear equations

14
SRTM-BFM
  • Parameter bounds must be determined based on
    regional analysis
  • Tight bounds cause poor fit and bias in some
    regions
  • Wide bounds may lead to long-tailed BP
    distribution and positive bias

15
SRTM-NNLS
  • Multilinear equation can be transformed to solve
    BP1 without division
  • Provides good-quality BP images when NNLS is used

16
SRTM-NNLS
BP image calculatedusing SRTM-NNLS
17
Parametric sinogram
  • Faster ( iterative ) reconstruction
  • Intrinsic heterogeneity
  • All linear models applicable

18
Parametric sinogram
DVR sinogram
DVR imageFBP reconstruction
19
Calculation on sinogram level
  1. Correct for physical decay
  2. Correct for frame lengths
  3. Model calculation as usual
  4. Reconstruction
  5. Divide pixel values by volume (if not done in
    reconstruction or calibration)
  6. Calibration (only with plasma input, and not even
    then for all parameters)
  7. Calculations with parameters after reconstruction

20
Parametric sinogram problems
  • Multiple-Time Graphical Analysis when linear
    phase starts?
  • Multilinear equations which model?
  • Reference input TAC pre-reconstruction needed

21
Parametric sinogrammore problems
  • Dynamic sinogram must be filtered before
    calculation avoid another filtering in
    reconstruction!
  • Requires full knowledge on raw data collection
    and processing steps

22
Parametric sinogram
  • In futureIterative reconstruction and model
    calculation combined

23
PROBLEMS
  • Noise induses bias in all linear methods for
    reversible uptake
  • Logan plot no satisfactory method for removing
    bias
  • Multilinear methods GLLS can not be applied to
    reference tissue models

24
More problems
  • SRTM can not be used for all tracers
  • Weights for fitting are not known
  • Partial volume error (PVE)may lead to
    artefactual second tissue compartment in
    reference region

25
More problems
  • Movement during scanning

DVR image without movement and after moving 3
frames 4 mm (2 pxls) upward
26
Movement during scanning
  • Complicated models are more sensitive to movement

Same simulation, but Logan plot computed with
variable line fit start time
27
Image filtering
  • Only working method to reduce bias in linear
    models
  • Resolution need not to be preserved if next
    analysis step is SPM or other brain averaging
    method
  • Biases may be cancelled out in calculation of
    occupancy maps

28
Cluster analysis
  • Resolution preserving smoothing for dynamic
    images
  • Automatic extraction of reference tissue curve
  • Extraction of curves with different kinetics
    Validation that selected model can fit them all

29
CONCLUSION
  • Problems image noise, patient movement and
    inconsistent input data
  • Until solved, use only simple models causing
    biases but less artefacts
  • Validation in animal models and in vitro is
    essential
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