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A novel technique for modeling susceptibility-based contrast mechanisms for arbitrary microvascular geometries: the finite perturber method.

机译:一种为任意微血管几何结构建立基于敏感性的对比机制的新技术:有限扰动法。

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摘要

Recently, we demonstrated that vessel geometry is a significant determinant of susceptibility-induced contrast in MRI. This is especially relevant for susceptibility-contrast enhanced MRI of tumors with their characteristically abnormal vessel morphology. In order to better understand the biophysics of this contrast mechanism, it is of interest to model how various factors, including microvessel morphology contribute to the measured MR signal, and was the primary motivation for developing a novel computer modeling approach called the Finite Perturber Method (FPM). The FPM circumvents the limitations of traditional fixed-geometry approaches, and enables us to study susceptibility-induced contrast arising from arbitrary microvascular morphologies in 3D, such as those typically observed with brain tumor angiogenesis. Here we describe this new modeling methodology and some of its applications. The excellent agreement of the FPM with theory and the extant susceptibility modeling data, coupled with its computational efficiency demonstrates its potential to transform our understanding of the factors that engender susceptibility contrast in MRI.
机译:最近,我们证明血管的几何形状是MRI中药敏性对比的重要决定因素。这对于具有特征性异常血管形态的肿瘤的敏感性对比增强MRI尤其重要。为了更好地了解这种对比机制的生物物理学,有必要对各种因素(包括微血管形态)如何影响测得的MR信号进行建模进行建模,这是开发一种名为Finite Perturber方法的新型计算机建模方法的主要动机( FPM)。 FPM规避了传统的固定几何方法的局限性,使我们能够研究3D中任意微血管形态(如脑肿瘤血管生成中通常观察到的形态)引起的磁化率对比。在这里,我们描述了这种新的建模方法及其一些应用。 FPM与理论和现有的磁化率建模数据极好的一致性,再加上其计算效率,证明了它有可能改变我们对MRI中磁化率对比因素的理解。

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