定量磁化率成像和R2*测量在多发性硬化症白质病变发展过程中的变化:髓鞘破坏、髓鞘碎片降解与清除以及铁蓄积
Quantitative Susceptibility Mapping and R2* Measured Changes during White Matter Lesion Development in Multiple Sclerosis: Myelin Breakdown, Myelin Debris Degradation and Removal, and Iron Accumulation.
作者信息
Zhang Y, Gauthier S A, Gupta A, Chen W, Comunale J, Chiang G C-Y, Zhou D, Askin G, Zhu W, Pitt D, Wang Y
机构信息
From the Department of Radiology (Y.Z., W.C., W.Z.), Tongji Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, China Departments of Radiology (Y.Z., A.G., J.C., G.C.-Y.C., D.Z., Y.W.).
Neurology (S.A.G.).
出版信息
AJNR Am J Neuroradiol. 2016 Sep;37(9):1629-35. doi: 10.3174/ajnr.A4825. Epub 2016 Jun 2.
BACKGROUND AND PURPOSE
Quantitative susceptibility mapping and R2* are sensitive to myelin and iron changes in multiple sclerosis lesions. This study was designed to characterize lesion changes on quantitative susceptibility mapping and R2* at various gadolinium-enhancement stages.
MATERIALS AND METHODS
This study included 64 patients with MS with different enhancing patterns in white matter lesions: nodular, shell-like, nonenhancing < 1 year old, and nonenhancing 1-3 years old. These represent acute, late acute, early chronic, and late chronic lesions, respectively. Susceptibility values measured on quantitative susceptibility mapping and R2* values were compared among the 4 lesion types. Their differences were assessed with a generalized estimating equation, controlling for Expanded Disability Status Scale score, age, and disease duration.
RESULTS
We analyzed 203 lesions: 80 were nodular-enhancing, of which 77 (96.2%) were isointense on quantitative susceptibility mapping; 33 were shell-enhancing, of which 30 (90.9%) were hyperintense on quantitative susceptibility mapping; and 49 were nonenhancing lesions < 1 year old and 41 were nonenhancing lesions 1-3 years old, all of which were hyperintense on quantitative susceptibility mapping. Their relative susceptibility/R2* values were 0.5 ± 4.4 parts per billion/-5.6 ± 2.9 Hz, 10.2 ± 5.4 parts per billion/-8.0 ± 2.6 Hz, 20.2 ± 7.8 parts per billion/-3.1 ± 2.3 Hz, and 33.2 ± 8.2 parts per billion/-2.0 ± 2.6 Hz, respectively, and were significantly different (P < .005).
CONCLUSIONS
Early active MS lesions with nodular enhancement show R2* decrease but no quantitative susceptibility mapping change, reflecting myelin breakdown; late active lesions with peripheral enhancement show R2* decrease and quantitative susceptibility mapping increase in the lesion center, reflecting further degradation and removal of myelin debris; and early or late chronic nonenhancing lesions show both quantitative susceptibility mapping and R2* increase, reflecting iron accumulation.
背景与目的
定量磁化率成像和R2对多发性硬化病变中的髓鞘和铁变化敏感。本研究旨在描述不同钆增强阶段定量磁化率成像和R2上病变的变化特征。
材料与方法
本研究纳入64例白质病变具有不同强化模式的多发性硬化患者:结节状、壳状、<1年的无强化病变以及1 - 3年的无强化病变。这些分别代表急性、亚急性、早期慢性和晚期慢性病变。比较4种病变类型在定量磁化率成像上测得的磁化率值和R2*值。采用广义估计方程评估它们的差异,并对扩展残疾状态量表评分、年龄和病程进行控制。
结果
我们分析了203个病变:80个为结节状强化,其中77个(96.2%)在定量磁化率成像上呈等信号;33个为壳状强化,其中30个(90.9%)在定量磁化率成像上呈高信号;49个为<1年的无强化病变,41个为1 - 3年的无强化病变,所有这些在定量磁化率成像上均呈高信号。它们的相对磁化率/R2*值分别为0.5±4.4十亿分之一/-5.6±2.9赫兹、10.2±5.4十亿分之一/-8.0±2.6赫兹、20.2±7.8十亿分之一/-3.1±2.3赫兹和33.2±8.2十亿分之一/-2.0±2.6赫兹,且差异有统计学意义(P <.005)。
结论
具有结节状强化的早期活动性多发性硬化病变显示R2降低但定量磁化率成像无变化,反映髓鞘破坏;具有周边强化的晚期活动性病变显示R2降低且病变中心定量磁化率成像增加,反映髓鞘碎片的进一步降解和清除;早期或晚期慢性无强化病变显示定量磁化率成像和R2*均增加,反映铁沉积。
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