首页> 外文会议>International conference on medical image computing and computer-assisted intervention;MICCAI 2010 >Cross-Visit Tumor Sub-segmentation and Registration with Outlier Rejection for Dynamic Contrast-Enhanced MRI Time Series Data
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Cross-Visit Tumor Sub-segmentation and Registration with Outlier Rejection for Dynamic Contrast-Enhanced MRI Time Series Data

机译:动态增强的MRI时间序列数据的跨视点肿瘤细分和异常值排除配准

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Clinical trials of anti-angiogenic and vascular-disrupting agents often use biomarkers derived from DCE-MRI, typically reporting whole-tumor summary statistics and so overlooking spatial parameter variations caused by tissue heterogeneity. We present a data-driven segmentation method comprising tracer-kinetic model-driven registration for motion correction, conversion from MR signal intensity to contrast agent concentration for cross-visit normalization, iterative principal components analysis for imputation of missing data and dimensionality reduction, and statistical outlier detection using the minimum covariance determinant to obtain a robust Mahalanobis distance. After applying these techniques we cluster in the principal components space using it-means. We present results from a clinical trial of a VEGF inhibitor, using time-series data selected because of problems due to motion and outlier time series. We obtained spatially-contiguous clusters that map to regions with distinct microvas-cular characteristics. This methodology has the potential to uncover localized effects in trials using DCE-MRI-based biomarkers.
机译:抗血管生成和血管破坏剂的临床试验通常使用衍生自DCE-MRI的生物标记物,通常报告整个肿瘤的汇总统计数据,因此可以忽略由组织异质性引起的空间参数变化。我们提出了一种数据驱动的分割方法,包括跟踪动力学模型驱动的配准以进行运动校正,从MR信号强度到造影剂浓度的转换以进行跨视点归一化,迭代主成分分析以估算缺失数据和降维,以及进行统计使用最小协方差行列式进行离群值检测以获得鲁棒的Mahalanobis距离。应用这些技术后,我们使用it-means将其聚集在主成分空间中。我们使用由于运动和异常时间序列引起的问题而选择的时间序列数据,提供了VEGF抑制剂临床试验的结果。我们获得了空间连续的簇,这些簇映射到具有不同微血管特征的区域。这种方法有可能在使用基于DCE-MRI的生物标记物的试验中揭示局部效应。

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