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A diffusion-compensated model for the analysis of DCE-MRI data: theory simulations and experimental results

机译:DCE-MRI数据分析的扩散补偿模型:理论仿真和实验结果

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摘要

Accurate quantification of pharmacokinetic parameters in dynamic contrast-enhanced (DCE) MRI may be affected by the passive diffusion of contrast agent (CA) within the tissue. By introducing an additional term into the standard Tofts-Kety (STK) model, we correct for the effects of CA diffusion. We first develop the theory describing a CA diffusion corrected STK model (DTK). The model is then tested in simulation with simple models of diffusion. The DTK model is also fit to 18 in vivo DCE-MRI acquisitions from murine models of cancer and results are compared to those from the STK model. The DTK model returned estimates with significantly lower error than the STK model (p≪0.001). In poorly-perfused (i.e., Ktrans≤0.05 min−1) regions the STK model returned unphysical ve values, while the DTK model estimated ve with less than 7% error in noise-free simulations. Results in vivo data revealed similar trends. For voxels with low Ktrans values and late peak concentration times the STK model returned ve estimates >1.0 in 40% of the voxels as compared to only 16% for the DTK model. The DTK model presented here shows promise in estimating accurate kinetic parameters in the presence of passive contrast agent diffusion.
机译:动态增强造影剂(DCE)MRI中药代动力学参数的准确定量可能会受到组织中造影剂(CA)被动扩散的影响。通过在标准Tofts-Kety(STK)模型中引入一个附加术语,我们可以校正CA扩散的影响。我们首先开发描述CA扩散校正的STK模型(DTK)的理论。然后使用简单的扩散模型在仿真中测试该模型。 DTK模型也适合从癌症鼠模型获得的18种体内DCE-MRI采集,并将结果与​​STK模型的结果进行比较。 DTK模型返回的估计误差比STK模型低得多(p≪0.001)。在灌注较差的区域(即,K trans ≤0.05min -1 )区域,STK模型返回的非物理ve值,而DTK模型估计的ve误差小于7%。在无噪声的模拟中。体内数据结果显示了相似的趋势。对于具有低K trans 值和晚期峰浓度时间的体素,STK模型在40%的体素中返回ve估计> 1.0,而DTK模型仅为16%。此处介绍的DTK模型显示了在存在被动造影剂扩散的情况下估算准确的动力学参数的希望。

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