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利用扩散磁共振成像评估视神经病理学:从小鼠到人类

Assessing optic nerve pathology with diffusion MRI: from mouse to human.

作者信息

Xu Junqian, Sun Shu-Wei, Naismith Robert T, Snyder Abraham Z, Cross Anne H, Song Sheng-Kwei

机构信息

Department of Neurology, Washington University in St Louis, St Louis, MO, USA.

出版信息

NMR Biomed. 2008 Nov;21(9):928-40. doi: 10.1002/nbm.1307.

Abstract

The optic nerve is often affected in patients with glaucoma and multiple sclerosis. Conventional MRI can detect nerve damage, but it does not accurately assess the underlying pathologies. Mean diffusivity and diffusion anisotropy indices derived from diffusion tensor imaging have been shown to be sensitive to a variety of central nervous system white matter pathologies. Despite being sensitive, the lack of specificity limits the ability of these measures to differentiate the underlying pathology. Directional (axial and radial) diffusivities, measuring water diffusion parallel and perpendicular to the axonal tracts, have been shown to be specific to axonal and myelin damage in mouse models of optic nerve injury, including retinal ischemia and experimental autoimmune encephalomyelitis. The progression of Wallerian degeneration has also been detected using directional diffusivities after retinal ischemia. However, translating these findings to human optic nerve is technically challenging. The current status of diffusion MRI of human optic nerve, including imaging sequences and protocols, is summarized herein. Despite the lack of a consensus among different groups on the optimal sequence or protocol, increased mean diffusivity and decreased diffusion anisotropy have been observed in injured optic nerve from patients with chronic optic neuritis. From different mouse models of optic nerve injuries to the emerging studies on patients with optic neuritis, directional diffusivities show great potential to be specific biomarkers for axonal and myelin injury.

摘要

青光眼和多发性硬化症患者的视神经常受影响。传统的磁共振成像(MRI)能够检测神经损伤,但无法准确评估潜在的病理状况。扩散张量成像得出的平均扩散率和扩散各向异性指数已被证明对多种中枢神经系统白质病变敏感。尽管这些指标具有敏感性,但其缺乏特异性限制了它们区分潜在病理状况的能力。在视神经损伤的小鼠模型中,包括视网膜缺血和实验性自身免疫性脑脊髓炎,测量与轴突束平行和垂直方向水扩散的定向(轴向和径向)扩散率已被证明对轴突和髓鞘损伤具有特异性。视网膜缺血后,利用定向扩散率也检测到了华勒氏变性的进展。然而,将这些研究结果应用于人类视神经在技术上具有挑战性。本文总结了人类视神经扩散MRI的现状,包括成像序列和方案。尽管不同研究团队对于最佳序列或方案尚未达成共识,但在慢性视神经炎患者的受损视神经中已观察到平均扩散率增加和扩散各向异性降低。从不同的视神经损伤小鼠模型到视神经炎患者的新兴研究,定向扩散率显示出作为轴突和髓鞘损伤特异性生物标志物的巨大潜力。

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