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双重扩散编码及其在生物医学成像中的应用。

Double diffusion encoding and applications for biomedical imaging.

机构信息

Champalimaud Research, Champalimaud Centre for the Unknown, Lisbon, Portugal.

Centre for Medical Image Computing and Dept. of Computer Science, University College London, London, UK.

出版信息

J Neurosci Methods. 2021 Jan 15;348:108989. doi: 10.1016/j.jneumeth.2020.108989. Epub 2020 Nov 1.

Abstract

Diffusion Magnetic Resonance Imaging (dMRI) is one of the most important contemporary non-invasive modalities for probing tissue structure at the microscopic scale. The majority of dMRI techniques employ standard single diffusion encoding (SDE) measurements, covering different sequence parameter ranges depending on the complexity of the method. Although many signal representations and biophysical models have been proposed for SDE data, they are intrinsically limited by a lack of specificity. Advanced dMRI methods have been proposed to provide additional microstructural information beyond what can be inferred from SDE. These enhanced contrasts can play important roles in characterizing biological tissues, for instance upon diseases (e.g. neurodegenerative, cancer, stroke), aging, learning, and development. In this review we focus on double diffusion encoding (DDE), which stands out among other advanced acquisitions for its versatility, ability to probe more specific diffusion correlations, and feasibility for preclinical and clinical applications. Various DDE methodologies have been employed to probe compartment sizes (Section 3), decouple the effects of microscopic diffusion anisotropy from orientation dispersion (Section 4), probe displacement correlations, study exchange, or suppress fast diffusing compartments (Section 6). DDE measurements can also be used to improve the robustness of biophysical models (Section 5) and study intra-cellular diffusion via magnetic resonance spectroscopy of metabolites (Section 7). This review discusses all these topics as well as important practical aspects related to the implementation and contrast in preclinical and clinical settings (Section 9) and aims to provide the readers a guide for deciding on the right DDE acquisition for their specific application.

摘要

扩散磁共振成像(dMRI)是目前最主要的非侵入性微观组织结构探测技术之一。大多数 dMRI 技术都采用标准的单扩散编码(SDE)测量方法,根据方法的复杂性,覆盖不同的序列参数范围。尽管已经提出了许多信号表示和生物物理模型来处理 SDE 数据,但它们本质上受到缺乏特异性的限制。先进的 dMRI 方法已经被提出,以提供超出 SDE 推断范围的额外微观结构信息。这些增强的对比可以在生物组织的特征化中发挥重要作用,例如在疾病(如神经退行性疾病、癌症、中风)、衰老、学习和发育等情况下。在本综述中,我们重点介绍双扩散编码(DDE),它在其他先进采集方法中脱颖而出,具有通用性、探测更特定扩散相关性的能力以及在临床前和临床应用中的可行性。已经采用了各种 DDE 方法来探测隔室大小(第 3 节)、分离微观扩散各向异性与方向分散的影响(第 4 节)、探测位移相关性、研究交换或抑制快速扩散隔室(第 6 节)。DDE 测量还可用于提高生物物理模型的稳健性(第 5 节),并通过代谢物的磁共振波谱研究细胞内扩散(第 7 节)。本综述讨论了所有这些主题以及与临床前和临床环境中的实施和对比相关的重要实际方面(第 9 节),旨在为读者提供一个指南,以决定针对其特定应用选择正确的 DDE 采集。

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