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急性视神经炎的系列磁化传递成像

Serial magnetization transfer imaging in acute optic neuritis.

作者信息

Hickman S J, Toosy A T, Jones S J, Altmann D R, Miszkiel K A, MacManus D G, Barker G J, Plant G T, Thompson A J, Miller D H

机构信息

NMR Research Unit, Department of Neuroinflammation, Institute of Neurology, University College London, Queen Square, London WC1N 3BG, UK.

出版信息

Brain. 2004 Mar;127(Pt 3):692-700. doi: 10.1093/brain/awh076. Epub 2004 Jan 21.

Abstract

In serial studies of multiple sclerosis lesions, reductions in magnetization transfer ratio (MTR) are thought to be due to demyelination and axonal loss, with later rises due to remyelination. This study followed serial changes in MTR in acute optic neuritis in combination with clinical and electrophysiological measurements to determine if the MTR changes over time mirror the picture in multiple sclerosis lesions, further validating MTR as a marker of tissue integrity. Twenty-nine patients were recruited who had acute optic neuritis for a median of 13 days (range 7-24 days) since the onset of visual symptoms. A clinical examination and measurement of visual evoked potentials (VEP) was performed on each patient. Their optic nerves were imaged with a fat-saturated fast spin echo (FSE) sequence and a magnetization transfer sequence. Twenty-one had multiple subsequent examinations over the course of 1 year. In addition, 27 control subjects had their optic nerves imaged up to three times over 1 year. A blinded observer segmented the optic nerves from the MTR maps. Lesions were defined on the acute FSE images and, from the coordinates, the ratio of mean lesion MTR : healthy nerve MTR (lesion ratio) was calculated for each dataset. The time-averaged mean MTR in control optic nerves was 47.7 per cent units (pu). In diseased optic nerves, baseline mean MTR was 47.3 pu, with a mean lesion ratio of 0.98. The diseased optic nerve MTR and lesion ratio declined over time with a nadir at about 240 days at a mean MTR value of 44.2 pu and mean lesion ratio of 0.91. Subsequently, diseased optic nerve MTR appeared to rise; after 1 year the diseased optic nerve mean MTR was 45.1 pu (mean lesion ratio 0.93), although the difference was not significant compared with the nadir value. For each 0.01 increase in time-averaged lesion ratio logMAR visual acuity recovery improved by 0.03 (95% CI, 0.002, 0.08, P = 0.02). Time-averaged VEP central field latency was shorter by 6.1 ms (95% CI 1.5, 10.7, P = 0.012) per 1 pu rise in time-averaged diseased optic nerve MTR. The early fall in diseased optic nerve MTR is consistent with demyelination and Wallerian degeneration of transected axons. The late nadir compared with studies of multiple sclerosis lesions may have been due to slow clearance of myelin debris. Remyelination may have influenced subsequent MTR changes. The observations support using MTR to monitor symptomatic demyelinating lesions.

摘要

在对多发性硬化症病灶的系列研究中,磁化传递率(MTR)的降低被认为是由于脱髓鞘和轴突损失,而后期的升高则是由于再髓鞘化。本研究追踪了急性视神经炎中MTR的系列变化,并结合临床和电生理测量,以确定MTR随时间的变化是否反映了多发性硬化症病灶的情况,从而进一步验证MTR作为组织完整性标志物的有效性。招募了29例自视觉症状发作以来急性视神经炎病程中位数为13天(范围7 - 24天)的患者。对每位患者进行了临床检查和视觉诱发电位(VEP)测量。用脂肪饱和快速自旋回波(FSE)序列和磁化传递序列对他们的视神经进行成像。其中21例在1年的病程中进行了多次后续检查。此外,27名对照受试者在1年中对视神经进行了多达3次成像。一名盲法观察者从MTR图中分割出视神经。在急性FSE图像上定义病灶,并根据坐标为每个数据集计算平均病灶MTR与健康神经MTR的比值(病灶比值)。对照视神经的时间平均MTR为47.7%单位(pu)。在患病视神经中,基线平均MTR为47.3 pu,平均病灶比值为0.98。患病视神经的MTR和病灶比值随时间下降,在约240天时达到最低点,平均MTR值为44.2 pu,平均病灶比值为0.91。随后,患病视神经的MTR似乎上升;1年后,患病视神经的平均MTR为45.1 pu(平均病灶比值0.93),尽管与最低点值相比差异不显著。时间平均病灶比值每增加0.01,logMAR视力恢复改善0.03(95%可信区间,0.002,0.08,P = 0.02)。时间平均患病视神经MTR每升高1 pu,时间平均VEP中心视野潜伏期缩短6.1毫秒(95%可信区间1.5,10.7,P = 0.012)。患病视神经MTR的早期下降与脱髓鞘和横断轴突的华勒氏变性一致。与多发性硬化症病灶研究相比,后期的最低点可能是由于髓鞘碎片清除缓慢。再髓鞘化可能影响了随后的MTR变化。这些观察结果支持使用MTR来监测有症状的脱髓鞘病灶。

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