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多发性硬化症患者脑萎缩的八年随访研究。

Eight-year follow-up study of brain atrophy in patients with MS.

作者信息

Fisher E, Rudick R A, Simon J H, Cutter G, Baier M, Lee J-C, Miller D, Weinstock-Guttman B, Mass M K, Dougherty D S, Simonian N A

机构信息

Whitaker Biomedical Imaging Laboratory, The Cleveland Clinic Foundation, OH 44195, USA.

出版信息

Neurology. 2002 Nov 12;59(9):1412-20. doi: 10.1212/01.wnl.0000036271.49066.06.

Abstract

OBJECTIVE

To characterize whole-brain atrophy in relapsing-remitting MS (RRMS) patients over an 8-year period. The specific goals of this study were to determine if brain atrophy is related to subsequent disability status and to identify MRI correlates of atrophy progression.

METHODS

A follow-up study was conducted to reassess patients from a phase III trial of interferon beta-1a (IFNbeta-1a) 8 years after randomization. Clinical and MRI data from 172 patients followed over 2 years in the original trial were used as baseline data. Follow-up data were obtained on 160 patients, including 134 patients with follow-up MRI examinations. Brain atrophy was estimated by automated calculation of brain parenchymal fraction. The relation between atrophy during the original trial and disability status at follow-up was determined. Correlations were also determined between lesion measurements from the original trial and the brain parenchymal fraction at follow-up.

RESULTS

Brain atrophy was correlated with subsequent disability status. Atrophy rate during the original trial was the most significant MRI predictor of disability status at follow-up. Brain atrophy at follow-up was related to lesion volumes measured during the original trial.

CONCLUSIONS

The relation between atrophy progression and subsequent neurologic disability status suggests that atrophy progression during RRMS is clinically relevant. Therefore, atrophy progression may be a useful marker for disease progression in clinical trials. The relation between lesions and subsequent atrophy indicates that brain atrophy may be related to focal tissue damage at earlier points in time, but important predisposing or other factors contributing to atrophy remain undefined.

摘要

目的

对复发缓解型多发性硬化症(RRMS)患者在8年期间的全脑萎缩情况进行特征描述。本研究的具体目标是确定脑萎缩是否与后续残疾状态相关,并识别萎缩进展的MRI相关因素。

方法

进行一项随访研究,在随机分组8年后对来自干扰素β-1a(IFNβ-1a)III期试验的患者进行重新评估。将原始试验中172例患者超过2年的临床和MRI数据用作基线数据。获取了160例患者的随访数据,其中134例患者进行了随访MRI检查。通过自动计算脑实质分数来估计脑萎缩情况。确定原始试验期间的萎缩与随访时残疾状态之间的关系。还确定了原始试验中的病灶测量值与随访时脑实质分数之间的相关性。

结果

脑萎缩与后续残疾状态相关。原始试验期间的萎缩率是随访时残疾状态最显著的MRI预测指标。随访时的脑萎缩与原始试验期间测量的病灶体积相关。

结论

萎缩进展与后续神经残疾状态之间的关系表明RRMS期间的萎缩进展具有临床相关性。因此,萎缩进展可能是临床试验中疾病进展的有用标志物。病灶与后续萎缩之间的关系表明,脑萎缩可能与早期的局灶性组织损伤有关,但导致萎缩的重要诱发因素或其他因素仍不明确。

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