TY - JOUR
T1 - Parametric methods for dynamic 11C-phenytoin PET studies
AU - Mansor, Syahir
AU - Yaqub, Maqsood
AU - Boellaard, Ronald
AU - Froklage, Femke E.
AU - De Vries, Anke
AU - Bakker, Esther D.M.
AU - Voskuyl, Rob A.
AU - Eriksson, Jonas
AU - Schwarte, Lothar A.
AU - Verbeek, Joost
AU - Windhorst, Albert D.
AU - Lammertsma, Adriaan A.
PY - 2017/3/1
Y1 - 2017/3/1
N2 - In this study, the performance of various methods for generating quantitative parametric images of dynamic 11C-phenytoin PET studies was evaluated. Methods: Double-baseline 60-min dynamic 11Cphenytoin PET studies, including online arterial sampling, were acquired for 6 healthy subjects. Parametric images were generated using Logan plot analysis, a basis function method, and spectral analysis. Parametric distribution volume (VT) and influx rate (K1) were compared with those obtained from nonlinear regression analysis of time-activity curves. In addition, global and regional test- retest (TRT) variability was determined for parametric K1 and VT values. Results: Biases in VT observed with all parametric methods were less than 5%. For K1, spectral analysis showed a negative bias of 16%. The mean TRT variabilities of VT and K1 were less than 10% for all methods. Shortening the scan duration to 45 min provided similar VT and K1 with comparable TRT performance compared with 60-min data. Conclusion: Among the various parametric methods tested, the basis function method provided parametric VT and K1 values with the least bias compared with nonlinear regression data and showed TRT variabilities lower than 5%, also for smaller volumeof- interest sizes (i.e., higher noise levels) and shorter scan duration.
AB - In this study, the performance of various methods for generating quantitative parametric images of dynamic 11C-phenytoin PET studies was evaluated. Methods: Double-baseline 60-min dynamic 11Cphenytoin PET studies, including online arterial sampling, were acquired for 6 healthy subjects. Parametric images were generated using Logan plot analysis, a basis function method, and spectral analysis. Parametric distribution volume (VT) and influx rate (K1) were compared with those obtained from nonlinear regression analysis of time-activity curves. In addition, global and regional test- retest (TRT) variability was determined for parametric K1 and VT values. Results: Biases in VT observed with all parametric methods were less than 5%. For K1, spectral analysis showed a negative bias of 16%. The mean TRT variabilities of VT and K1 were less than 10% for all methods. Shortening the scan duration to 45 min provided similar VT and K1 with comparable TRT performance compared with 60-min data. Conclusion: Among the various parametric methods tested, the basis function method provided parametric VT and K1 values with the least bias compared with nonlinear regression data and showed TRT variabilities lower than 5%, also for smaller volumeof- interest sizes (i.e., higher noise levels) and shorter scan duration.
KW - 11C-phenytoin
KW - PET quantification
KW - Parametric kinetic modeling
KW - Test-retest variability
UR - http://www.scopus.com/inward/record.url?scp=85014858701&partnerID=8YFLogxK
U2 - https://doi.org/10.2967/jnumed.116.178707
DO - https://doi.org/10.2967/jnumed.116.178707
M3 - Article
C2 - 27660142
SN - 0161-5505
VL - 58
SP - 479
EP - 483
JO - Journal of nuclear medicine
JF - Journal of nuclear medicine
IS - 3
ER -