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与纳武单抗相关的进行性多灶性白质脑病中的免疫重建炎症综合征。

Immune reconstitution inflammatory syndrome in natalizumab-associated PML.

机构信息

Department of Neurology, Johns Hopkins School of Medicine, Baltimore, MD, USA.

出版信息

Neurology. 2011 Sep 13;77(11):1061-7. doi: 10.1212/WNL.0b013e31822e55e7. Epub 2011 Aug 10.

DOI:10.1212/WNL.0b013e31822e55e7
PMID:21832229
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3174071/
Abstract

OBJECTIVE

To study the outcome of patients with multiple sclerosis (MS) and with natalizumab-associated progressive multifocal leukoencephalopathy (PML) and immune reconstitution inflammatory syndrome (IRIS).

METHODS

MedWatch reports from Biogen-Idec (manufacturer of natalizumab, Tysabri(®)) were reviewed which comprised all 42 cases of natalizumab-related PML cases since its reintroduction until March 2010.

RESULTS

All except 2 patients with natalizumab-related PML were managed by discontinuation of natalizumab and plasmapheresis/immunoadsorption (PLEX/IA). Seventeen patients had contrast enhancement of PML lesions on neuroimaging at the time of diagnosis before withdrawal/removal of natalizumab (early-PML-IRIS) and 23 patients developed contrast enhancement only after withdrawal/removal of natalizumab (late-PML-IRIS). All patients developed IRIS. IRIS was defined as worsening of neurologic deficits during the immune reconstitution following discontinuation of natalizumab, corroborated by inflammatory changes on neuroimaging. Following PLEX/IA, JC viral load in CSF increased by >10 fold in those with early-PML-IRIS but <2 fold in late-PML-IRIS. IRIS developed earlier and was more severe in early-PML-IRIS (p < 0.05). At the last follow-up, all patients had worse EDSS scores but this was higher in patients with early-PML-IRIS compared to those with late-PML-IRIS (p > 0.05). Mortality was comparable between the 2 groups, 29.4 ± 11% vs 21.7 ± 8.8%. Corticosteroid therapy during IRIS was associated with better Expanded Disability Status Scale outcome, p < 0.05.

CONCLUSION

Early immunologic rebound in natalizumab-associated PML has worse survival and neurologic outcome. PLEX/IA may accelerate IRIS and its impact on the final outcome is unclear. Corticosteroid therapy provides a modest benefit and needs to be systemically studied in a controlled manner in the management of natalizumab-associated PML-IRIS.

摘要

目的

研究多发性硬化症(MS)患者和与那他珠单抗相关进行性多灶性白质脑病(PML)和免疫重建炎症综合征(IRIS)的患者的结局。

方法

对 Biogen-Idec(那他珠单抗制造商,Tysabri®)的 MedWatch 报告进行了回顾,这些报告包括自那他珠单抗重新引入以来至 2010 年 3 月期间所有 42 例那他珠单抗相关 PML 病例。

结果

除 2 例那他珠单抗相关 PML 患者外,所有患者均通过停用那他珠单抗和血浆置换/免疫吸附(PLEX/IA)进行治疗。在停用/去除那他珠单抗之前(早期-PML-IRIS),17 例 PML 患者神经影像学检查显示 PML 病变有对比增强,而 23 例患者仅在停用/去除那他珠单抗后出现对比增强(晚期-PML-IRIS)。所有患者均出现 IRIS。IRIS 定义为停用那他珠单抗后免疫重建期间神经功能缺损恶化,并伴有神经影像学上的炎症改变。在 PLEX/IA 后,早期-PML-IRIS 患者的 CSF 中 JC 病毒载量增加了>10 倍,而晚期-PML-IRIS 患者则增加了<2 倍。早期-PML-IRIS 患者的 IRIS 更早且更严重(p<0.05)。在最后一次随访时,所有患者的 EDSS 评分均更差,但早期-PML-IRIS 患者的评分高于晚期-PML-IRIS 患者(p>0.05)。两组死亡率相当,分别为 29.4%±11%和 21.7%±8.8%。IRIS 期间使用皮质类固醇治疗与更好的扩展残疾状况量表(EDSS)结局相关,p<0.05。

结论

那他珠单抗相关 PML 中的早期免疫反弹具有更差的生存和神经功能结局。PLEX/IA 可能加速 IRIS,但其对最终结局的影响尚不清楚。皮质类固醇治疗提供了适度的益处,需要在纳他珠单抗相关 PML-IRIS 的管理中以系统的方式进行对照研究。

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