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Quasi-Conformal Technique for Integrating and Validating Myocardial Tissue Characterization in MRI with Ex-Vivo Human Histological Data

机译:准共形技术,用于整合和验证具有先前人类组织学数据的MRI中的心肌组织特征

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Ventricular tachycardia caused by a circuit of re-entry is one of the most critical arrhythmias. It is usually related with heterogeneous scar regions where slow velocity of conduction tissue is mixed with non-conductive tissue, creating pathways (CC) responsible for the tachycardia. Pre-operative DE-MRI can provide information on myocardial tissue viability and then improve therapy planning. However, the current DE-MRI resolution is not sufficient for identifying small CCs and therefore they have to be identified during the intervention, which requires considerable operator experience. In this work, we studied the relationship of histological data (with 10μm resolution), with in-vivo DE-MRI pixel intensities (PI) of one human heart. Integrating multi-modal data provided by different nature (in- vs. ex-vivo; 3D volume vs. 2D slices) is not straightforward and requires a robust integration pipeline. The main purpose of this work, is to develop a new technique for integrating histological information into the corresponding DE-MRI one. The proposed quasi-conformal mapping technique (QCM) integration were compared with state-of-the-art registration techniques (affine and non-rigid) on a benchmark of 418 synthetically generated datasets showing a more robust results. We used the QCM to quantitatively compare DE-MRI PI with the percentage of fibrosis extracted from histology. We show a positive correlation between the DE-MRI PI and the percentage of fibrosis extracted from histology (r = 0.97; p < 0.0001). Furthermore, we found a significant amount of viable tissue (up to 50%) in areas commonly defined as core zone in DE-MRI (PI level > 60% of the maximum intensity value).
机译:再入回路引起的室性心动过速是最严重的心律不齐之一。它通常与异质疤痕区域有关,在异质疤痕区域中,传导组织的慢速速度与非传导性组织混合,从而形成负责心动过速的途径(CC)。术前DE-MRI可以提供有关心肌组织生存力的信息,然后改善治疗计划。但是,当前的DE-MRI分辨率不足以识别小型CC,因此必须在干预过程中将其识别出来,这需要相当多的操作员经验。在这项工作中,我们研究了组织学数据(分辨率为10μm)与一个人心脏的体内DE-MRI像素强度(PI)的关系。集成不同性质(体内或体外; 3D体积与2D切片)提供的多模式数据并非易事,需要强大的集成管道。这项工作的主要目的是开发一种将组织学信息整合到相应的DE-MRI中的新技术。在以418个综合生成的数据集为基准的基础上,将拟议的准保形映射技术(QCM)集成与最新的注册技术(仿射和非刚性)进行了比较。我们使用QCM对DE-MRI PI与从组织学中提取的纤维化百分比进行定量比较。我们显示DE-MRI PI与组织学提取的纤维化百分比呈正相关(r = 0.97; p <0.0001)。此外,我们在通常被定义为DE-MRI核心区域的区域(PI水平>最大强度值的60%)中发现了大量的活组织(高达50%)。

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