Comparative study of methods for determining vascular permeability and blood volume in human gliomas

Abstract

Purpose To characterize human gliomas using T₁‐weighted dynamic contrast‐enhanced MRI (DCE‐MRI), and directly compare three pharmacokinetic analysis techniques: a conventional established technique and two novel techniques that aim to reduce erroneous overestimation of the volume transfer constant between plasma and the extravascular extracellular space (EES) (K^trans) in areas of high blood volume. Materials and Methods Eighteen patients with high‐grade gliomas underwent DCE‐MRI. Three kinetic models were applied to estimate K^trans and fractional blood plasma volume (v_p). We applied the Tofts and Kermode (TK) model without arterial input function (AIF) estimation, the TK model modified to include v_p and AIF estimation (mTK), and a “first pass” variant of the TK model (FP). Results K_TK values were considerably higher than K_mTK and K_FP values (P < 0.001). K_mTK and K_FP were more comparable and closely correlated (ρ = 0.744), with K_mTK generally higher than K_FP (P < 0.001). Estimates of v_p(mTK) and v_p(FP) also showed a significant difference (P < 0.001); however, these values were very closely correlated (ρ = 0.901). K_TK parameter maps showed “pseudopermeability” effects displaying numerous vessels. These were not visualized on K_mTK and K_FP maps but appeared on the corresponding v_p maps, indicating a failure of the TK model in commonly occurring vascular regions. Conclusion Both of the methods that incorporate a measured AIF and an estimate of v_p provide similar pathophysiological information and avoid erroneous overestimation of K^trans in areas of significant vessel density, and thus allow a more accurate estimation of endothelial permeability. J. Magn. Reson. Imaging 2004;20:748–757.