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亨廷顿舞蹈症的扩散成像:全面综述

Diffusion imaging in Huntington's disease: comprehensive review.

作者信息

Estevez-Fraga Carlos, Scahill Rachael, Rees Geraint, Tabrizi Sarah J, Gregory Sarah

机构信息

Huntington's Disease Centre, Department of Neurodegenerative Disease, UCL Queen Square Institute of Neurology, University College London, London, UK.

Wellcome Centre for Neuroimaging, University College London, London, UK.

出版信息

J Neurol Neurosurg Psychiatry. 2020 Oct 8;92(1):62-9. doi: 10.1136/jnnp-2020-324377.

Abstract

Huntington's disease (HD) is a monogenic disorder with 100% penetrance. With the advent of genetic testing in adults, disease-related, structural brain changes can be investigated from the earliest, premorbid stages of HD. While examining macrostructural change characterises global neuronal damage, investigating microstructural alterations provides information regarding brain organisation and its underlying biological properties. Diffusion MRI can be used to track the progression of microstructural anomalies in HD decades prior to clinical disease onset, providing a greater understanding of neurodegeneration. Multiple approaches, including voxelwise, region of interest and tractography, have been used in HD cohorts, showing a centrifugal pattern of white matter (WM) degeneration starting from deep brain areas, which is consistent with neuropathological studies. The corpus callosum, longer WM tracts and areas that are more densely connected, in particular the sensorimotor network, also tend to be affected early during premanifest stages. Recent evidence supports the routine inclusion of diffusion analyses within clinical trials principally as an additional measure to improve understanding of treatment effects, while the advent of novel techniques such as multitissue compartment models and connectomics can help characterise the underpinnings of progressive functional decline in HD.

摘要

亨廷顿舞蹈症(HD)是一种具有100%外显率的单基因疾病。随着成人基因检测的出现,可以从HD最早的发病前阶段开始研究与疾病相关的大脑结构变化。虽然检查宏观结构变化可表征整体神经元损伤,但研究微观结构改变能提供有关脑组织及其潜在生物学特性的信息。扩散磁共振成像(MRI)可用于追踪HD临床疾病发作前数十年微观结构异常的进展情况,有助于更深入地了解神经退行性变。HD队列研究采用了多种方法,包括体素分析、感兴趣区域分析和纤维束成像,结果显示白质(WM)变性呈离心模式,始于深部脑区,这与神经病理学研究结果一致。胼胝体、较长的WM纤维束以及连接更密集的区域,特别是感觉运动网络,在临床症状出现前阶段也往往较早受到影响。最近的证据支持在临床试验中常规纳入扩散分析,主要作为一种辅助手段,以更好地理解治疗效果,而多组织隔室模型和连接组学等新技术的出现,有助于阐明HD进行性功能衰退的潜在机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1620/7803908/95efc67da145/jnnp-2020-324377f01.jpg

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