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Towards accurate and precise T1 and extracellular volume mapping in the myocardium: a guide to current pitfalls and their solutions

机译:迈向心肌中精确和精确的T1和细胞外体积定位:当前陷阱及其解决方案的指南

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摘要

Mapping of the longitudinal relaxation time (T 1) and extracellular volume (ECV) offers a means of identifying pathological changes in myocardial tissue, including diffuse changes that may be invisible to existing T 1-weighted methods. This technique has recently shown strong clinical utility for pathologies such as Anderson-Fabry disease and amyloidosis and has generated clinical interest as a possible means of detecting small changes in diffuse fibrosis; however, scatter in T 1 and ECV estimates offers challenges for detecting these changes, and bias limits comparisons between sites and vendors. There are several technical and physiological pitfalls that influence the accuracy (bias) and precision (repeatability) of T 1 and ECV mapping methods. The goal of this review is to describe the most significant of these, and detail current solutions, in order to aid scientists and clinicians to maximise the utility of T 1 mapping in their clinical or research setting. A detailed summary of technical and physiological factors, issues relating to contrast agents, and specific disease-related issues is provided, along with some considerations on the future directions of the field.
机译:纵向舒张时间(T 1)和细胞外体积(ECV)的映射提供了一种识别心肌组织病理变化的方法,包括现有的T 1加权方法可能看不到的弥散变化。这项技术最近显示出对诸如安德森-法布里(Anderson-Fabry)病和淀粉样变性等病理学的强大临床效用,并已引起了临床兴趣,作为检测弥漫性纤维化微小变化的可能手段。但是,T 1和ECV估计值的分散为检测这些变化带来了挑战,并且偏差限制了站点和供应商之间的比较。有一些技术和生理上的陷阱会影响T 1和ECV映射方法的准确性(偏差)和准确性(可重复性)。这篇综述的目的是描述这些方法中最重要的方法,并详细介绍当前的解决方案,以帮助科学家和临床医生在其临床或研究环境中最大程度地利用T 1作图。提供了技术和生理因素,与造影剂有关的问题以及与疾病有关的特定问题的详细摘要,以及对该领域未来方向的一些考虑。

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