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Dynamic Contrast-Enhanced Imaging and Analysis at High Spatial Resolution of MCF7 Human Breast Tumors

机译:MCF7人乳腺肿瘤高空间分辨率的动态对比度增强成像和分析

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摘要

High resolution, dynamic GdDTPA-enhanced images of MCF7 human breast tumors in immunodeficient mice were analyzed at pixel resolution. The analysis, based on a physiological model, was performed by applying a nonlinear least-square algorithm using a color coded scale. The final output mapped at pixel resolution capillary permeability times surface area and fraction of extracellular volume, for each tumor slice. In addition, the output included assessment of the fit to the model by determining the proportion of variability (R2) for each pixel. The spatial variation in theR2values served to identify regions where the predominant mechanism of enhancement was leakage from the intravascular volume to the extracellular volume (R2close to 1). In regions with lowR2other mechanisms of enhancement appear to be dominating presumably diffusion within the extracellular space. As expected, in necrotic regions lacking microcapillaries and identified by analyzingT2-weighted images of the same tumors, the model failed to fit the dynamic contrast enhanced data. The heterogeneous distribution of the determined pathophysiological features demonstrates the importance of recording and analyzing breast tumor images at high spatial resolution.
机译:在像素分辨率下分析了高分辨率,在免疫缺陷小鼠中的MCF7人乳腺肿瘤的动态GDDTPA增强图像。通过使用颜色编码刻度应用非线性最小二乘算法来执行基于生理模型的分析。对于每种肿瘤切片,最终输出映射到每个肿瘤切片的像素分辨率透析毛细血管型次数和细胞外体积的一部分。另外,输出包括通过确定每个像素的变异性(R2)的比例来评估拟合到模型。 THEVALUES的空间变化用于鉴定从血管内体积与细胞外体积的增强机制泄漏的区域(R 2至1)。在具有低温的区域中,增强机制似乎是在细胞外空间内的扩散占据主导地位。正如预期的那样,在缺乏微毛细血管的坏死区域并通过相同肿瘤的分析重量图像识别,模型无法符合动态对比度增强数据。确定的病理物理学特征的异质分布证明了在高空间分辨率下记录和分析乳腺肿瘤图像的重要性。

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