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早期多发性硬化症中的轴突损伤是不可逆的,且与疾病的短期进展无关。

Axonal injury in early multiple sclerosis is irreversible and independent of the short-term disease evolution.

作者信息

Rovaris M, Gambini A, Gallo A, Falini A, Ghezzi A, Benedetti B, Sormani M P, Martinelli V, Comi G, Filippi M

机构信息

Neuroimaging Research Unit, Scientific Institute and University Ospedale San Raffaele, Milan, Italy.

出版信息

Neurology. 2005 Nov 22;65(10):1626-30. doi: 10.1212/01.wnl.0000184493.06254.a6.

Abstract

OBJECTIVE

To define the nature and the temporal evolution of neuronal/axonal injury in patients at the earliest clinical stage of multiple sclerosis (MS), using whole brain N-acetylaspartate (WBNAA) proton MR spectroscopy (1H-MRS).

METHODS

Thirty-five patients at presentation with clinically isolated syndromes (CIS) and MRI evidence of disease dissemination in space were studied. The following scans of the brain were acquired within 3 months from the onset of the disease and after 12 months: 1) dual-echo; 2) WBNAA 1H-MRS; 3) pre- and postcontrast T1-weighted. The same scans were obtained in 12 age-matched healthy subjects, without contrast administration. In patients, conventional MRI scans were also repeated 3 months after the first scanning session, to assess the presence of early disease dissemination in time (DIT).

RESULTS

Over the study period, 24 patients showed MRI evidence of disease DIT, thus fulfilling the criteria for a diagnosis of MS. The average WBNAA amount was lower in CIS patients than in controls both at baseline (13.7 vs 16.9 mM, p < 0.001) and at 1-year follow-up (12.6 vs 16.2 mM, p < 0.001), but the average yearly percentage change of WBNAA did not differ between the two groups. No MRI or 1H-MRS quantities were significantly associated with the disease DIT over the study period.

CONCLUSION

Irreversible brain damage associated with axonal dysfunction occurs at a very early stage in patients with clinically isolated syndromes, but it does not seem to be related with the disease evolution in the subsequent short-term period.

摘要

目的

使用全脑 N - 乙酰天门冬氨酸(WBNAA)质子磁共振波谱(1H - MRS),在多发性硬化症(MS)的最早临床阶段确定患者神经元/轴突损伤的性质和时间演变。

方法

对 35 例表现为临床孤立综合征(CIS)且有空间疾病播散的 MRI 证据的患者进行研究。在疾病发作后 3 个月内及 12 个月后进行以下脑部扫描:1)双回波;2)WBNAA 1H - MRS;3)增强前后的 T1 加权像。在 12 名年龄匹配的健康受试者中进行相同扫描,不使用造影剂。在患者中,首次扫描后 3 个月也重复进行常规 MRI 扫描,以评估早期时间上的疾病播散(DIT)情况。

结果

在研究期间,24 例患者显示出疾病 DIT 的 MRI 证据,从而符合 MS 诊断标准。CIS 患者的平均 WBNAA 量在基线时(13.7 对 16.9 mM,p < 0.001)和 1 年随访时(12.6 对 16.2 mM,p < 0.001)均低于对照组,但两组间 WBNAA 的平均年变化百分比无差异。在研究期间,没有 MRI 或 1H - MRS 量与疾病 DIT 显著相关。

结论

与轴突功能障碍相关的不可逆脑损伤在临床孤立综合征患者的极早期就已发生,但在随后的短期内似乎与疾病进展无关。

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