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Breast dispersion imaging using undersampled rapid dynamic contrast-enhanced MRI

机译:使用欠采样的快速动态对比度增强MRI使用乳房分散成像

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Purpose: Rapid dynamic contrast-enhanced magnetic resonance imaging (DCE-MRI) enables the tracking of rapid contrast accumulation, which is an important indication for cancer angiogenesis. Conventional pharmacokinetic models focusing on evaluating microvascular perfusion have limited abilities in detecting these features. In this work, we explore the performance of a novel dispersion pharmacokinetic model in discriminating benign and malignant tumor tissues and compare that with conventional non-dispersion methods. Methods: According to the convective-dispersion equation, the microvascular architecture changes can be explained using dispersion parameters. The dispersion maps are estimated by fitting a modified local density random walk (mLDRW) dispersion model to the concentration-time curves (CTC) in a voxel-by-voxel level. Measurement of an arterial input function is no longer required. We compare the fitting performance of this model with three classic non-dispersion pharmacokinetic models (i.e., Tofts, extended Tofts and comprehensive 2 compartment exchange model (2CXM)) that are commonly used for tumor characterization. The performance in discriminating benign and malignant tumors for dispersion and non-dispersion parameter maps are compared using receiver operating characteristic curve (ROC). Evaluation study is performed on 60 tumors that are acquired from 37 patients. Results: The goodness-of-fit is significantly improved with mLDRW model. Comparing to non-dispersion parameter maps, the dispersion related parameter maps provide the highest area under the ROC (AUC) of 0.96 with a sensitivity of 84.7 and specificity of 90.5. Conclusion: In this work, we provide a new window to investigate the physiology of breast tumor microcirculation through the estimation of intravascular dispersion property. The dispersion related parameter demonstrates superior performance in discriminating benign and malignant tumors.
机译:目的:快速动态对比度增强磁共振成像(DCE-MRI)能够跟踪快速对比度积累,这是癌症血管生成的重要迹象。关注评估微血管灌注的常规药代动力学模型具有检测这些特征的有限能力。在这项工作中,我们探讨了一种新型分散药代动力学模型在辨别良性和恶性肿瘤组织中的性能,并与常规的非分散方法进行比较。方法:根据对流分散方程,可以使用色散参数来解释微血管架构的变化。通过将改性的局部密度随机步行(MLDRW)分散模型拟合到体素水平中的浓度 - 时间曲线(CTC)来估计分散图。不再需要测量动脉输入功能。我们将该模型的拟合性能与三种经典的非分散药代动画片(即礼帽,延长的Tofts和全面的2个隔室交换模型(2cxm))进行比较,这些模型通常用于肿瘤表征。使用接收器操作特性曲线(ROC)比较用于分散和非分散参数映射的区分良恶性肿瘤的性能。评估研究是在37名患者获得的60种肿瘤上进行的。结果:使用MLDRW模型显着改善了健康。与非色散参数映射相比,色散相关参数图提供0.96的ROC(AUC)下的最高面积,灵敏度为84.7和90.5的特异性。结论:在这项工作中,我们提供了一种新的窗口,以通过估计血管内分散性能来研究乳腺肿瘤微循环的生理学。分散相关参数在歧视良性和恶性肿瘤中表现出优异的性能。

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