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多发性硬化症:阿仑单抗治疗后视觉系统的结构和功能完整性。

Multiple sclerosis: structural and functional integrity of the visual system following alemtuzumab therapy.

机构信息

Sydney Neuroimaging Analysis Centre, Camperdown, New South Wales, Australia.

Brain and Mind Centre, The University of Sydney, Camperdown, New South Wales, Australia.

出版信息

J Neurol Neurosurg Psychiatry. 2021 Dec;92(12):1319-1324. doi: 10.1136/jnnp-2021-326164. Epub 2021 Jun 29.

DOI:10.1136/jnnp-2021-326164
PMID:34187865
Abstract

OBJECTIVE

To investigate potential neuroprotective and pro-remyelinating effects of alemtuzumab in multiple sclerosis (MS), using the visual pathway as a model.

METHODS

We monitored clinical, multifocal visual evoked potential (mfVEP) and MRI outcomes in 30 patients commencing alemtuzumab for relapsing MS, and a reference group of 20 healthy controls (HCs), over 24 months. Change in mfVEP latency was the primary endpoint; change in optic radiation (OR) lesion diffusion metrics and Mars letter contrast sensitivity over the course of the study were secondary endpoints.

RESULTS

In patients, we observed a mean shortening of mfVEP latency of 1.21 ms over the course of the study (95% CI 0.21 to 2.21, p=0.013), not altered by correction for age, gender, disease duration or change in OR T2 lesion volume. Mean mfVEP latency in the HC group increased over the course of the study by 0.72 ms (not significant). Analysis of chronic OR T2 lesions (patients) showed an increase in normalised fractional anisotropy and axial diffusivity between baseline and 24 months (both p<0.01). Mean Mars letter contrast sensitivity was improved at 24 months vs baseline (p<0.001), and driven by an early improvement, in both patients and HC.

CONCLUSION

We found evidence of partial lesion remyelination after alemtuzumab therapy, indicating either natural restoration in the context of a 'permissive' local milieu; or potentially an independent, pro-reparative mechanism of action. The visual system presents a unique opportunity to study function-structure specific effects of therapy and inform the design of future phase 2 MS remyelination trials.

摘要

目的

以视觉通路为模型,研究阿仑单抗(alemtuzumab)在多发性硬化(MS)中的潜在神经保护和促髓鞘再生作用。

方法

我们在 24 个月的时间里,监测了 30 名开始接受阿仑单抗治疗的复发性 MS 患者和 20 名健康对照者(HCs)的临床、多焦视觉诱发电位(mfVEP)和 MRI 结果。mfVEP 潜伏期的变化是主要终点;研究过程中视辐射(OR)病变弥散指标和 Mars 字母对比敏感度的变化是次要终点。

结果

在患者中,我们观察到 mfVEP 潜伏期在研究过程中平均缩短了 1.21 毫秒(95%CI 0.21 至 2.21,p=0.013),但不受年龄、性别、疾病持续时间或 OR T2 病变体积变化的校正影响。HC 组的 mfVEP 潜伏期在研究过程中平均增加了 0.72 毫秒(无统计学意义)。对慢性 OR T2 病变(患者)的分析显示,正常化各向异性分数和轴向弥散度在基线和 24 个月之间增加(均 p<0.01)。与基线相比,24 个月时的平均 Mars 字母对比敏感度提高(p<0.001),这是由患者和 HCs 早期改善引起的。

结论

我们发现阿仑单抗治疗后有部分病变发生髓鞘再生的证据,这表明在“允许”的局部环境中存在自然恢复;或者可能存在独立的促修复作用机制。视觉系统为研究治疗的功能-结构特异性效应提供了一个独特的机会,并为未来的多发性硬化症髓鞘再生 2 期试验设计提供了信息。

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