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多发性硬化症中的病灶异质性:关于T1加权图像表现、T1弛豫时间与代谢物浓度之间关系的研究

Lesion heterogeneity in multiple sclerosis: a study of the relations between appearances on T1 weighted images, T1 relaxation times, and metabolite concentrations.

作者信息

Brex P A, Parker G J, Leary S M, Molyneux P D, Barker G J, Davie C A, Thompson A J, Miller D H

机构信息

NMR Research Unit, 6th floor, Institute of Neurology, University College London, Queen Square, London WC1N 3BG, UK.

出版信息

J Neurol Neurosurg Psychiatry. 2000 May;68(5):627-32. doi: 10.1136/jnnp.68.5.627.

Abstract

OBJECTIVES

Multiple sclerosis lesions appear as areas of high signal on T2 weighted MRI. A proportion of these lesions, when viewed on T1 weighted MRI, appear hypointense compared with surrounding white matter. These hypointense T1 lesions are thought to represent areas of greater tissue damage compared with the more non-specific, total T2 lesion load. This study aimed to better characterise the properties of high signal T2 lesions with differing appearances on T1 weighted MRI using quantitative MR techniques.

METHODS

Eleven patients with secondary progressive multiple sclerosis were studied. Two high signal T2 lesions were selected from each patient-one of which appeared hypointense and one isointense on a T1 weighted image. A voxel was positioned around each lesion and for this volume of brain the metabolite concentrations were estimated using proton MR spectroscopy ((1)H-MRS) and the T1 relaxation time within each voxel calculated from a T1 map generated using a multislice technique.

RESULTS

Compared with isointense T1 lesions, hypointense T1 lesions exhibited a significantly lower absolute concentration of N-acetyl derived metabolites (tNAA) and a significantly higher absolute concentration of myo-inositol (Ins). T1 relaxation time correlated significantly with both tNAA (r=-0.8, p < 0.001) and Ins (r=0.5, p=0. 012). There was no correlation between T1 relaxation times and creatine/phosphocreatine or choline containing compounds.

CONCLUSIONS

Prolonged T1 relaxation times seem to reflect the severity of axonal damage or dysfunction (inferred by a low tNAA) and possibly also gliosis (inferred by a high Ins) in chronic multiple sclerosis lesions.

摘要

目的

多发性硬化病灶在T2加权磁共振成像(MRI)上表现为高信号区。在T1加权MRI上观察时,这些病灶中有一部分与周围白质相比呈低信号。与更具非特异性的总T2病灶负荷相比,这些T1低信号病灶被认为代表了更大的组织损伤区域。本研究旨在使用定量磁共振技术更好地表征在T1加权MRI上具有不同表现的T2高信号病灶的特性。

方法

对11例继发进展型多发性硬化患者进行研究。从每位患者中选取两个T2高信号病灶——其中一个在T1加权图像上呈低信号,另一个呈等信号。在每个病灶周围放置一个体素,并针对该脑体积使用质子磁共振波谱((1)H-MRS)估计代谢物浓度,并根据使用多层技术生成的T1图计算每个体素内的T1弛豫时间。

结果

与T1等信号病灶相比,T1低信号病灶的N-乙酰衍生代谢物(总N-乙酰天门冬氨酸,tNAA)绝对浓度显著降低,肌醇(Ins)绝对浓度显著升高。T1弛豫时间与tNAA(r=-0.8,p<0.001)和Ins(r=0.5,p=0.012)均显著相关。T1弛豫时间与肌酸/磷酸肌酸或含胆碱化合物之间无相关性。

结论

在慢性多发性硬化病灶中,延长的T1弛豫时间似乎反映了轴突损伤或功能障碍的严重程度(由低tNAA推断),也可能反映了胶质增生(由高Ins推断)。

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