Department of Neurology, Washington University in St Louis, Saint Louis, MO 63110, USA.
Lancet Neurol. 2010 Apr;9(4):438-46. doi: 10.1016/S1474-4422(10)70028-4.
Treatment of multiple sclerosis with natalizumab is complicated by rare occurrence of progressive multifocal leukoencephalopathy (PML). Between July, 2006, and November, 2009, there were 28 cases of confirmed PML in patients with multiple sclerosis treated with natalizumab. Assessment of these clinical cases will help to inform future therapeutic judgments and improve the outcomes for patients.
The risk of PML increases with duration of exposure to natalizumab over the first 3 years of treatment. No new cases occurred during the first two years of natalizumab marketing but, by the end of November, 2009, 28 cases had been confirmed, of which eight were fatal. The median treatment duration to onset of symptoms was 25 months (range 6-80 months). The presenting symptoms most commonly included changes in cognition, personality, and motor performance, but several cases had seizures as the first clinical event. Although PML has developed in patients without any previous use of disease-modifying therapies for multiple sclerosis, previous therapy with immunosuppressants might increase risk. Clinical diagnosis by use of MRI and detection of JC virus in the CSF was established in all but one case. Management of PML has routinely used plasma exchange (PLEX) or immunoabsorption to hasten clearance of natalizumab and shorten the period in which natalizumab remains active (usually several months). Exacerbation of symptoms and enlargement of lesions on MRI have occurred within a few days to a few weeks after PLEX, indicative of immune reconstitution inflammatory syndrome (IRIS). This syndrome seems to be more common and more severe in patients with natalizumab-associated PML than it is in patients with HIV-associated PML. WHERE NEXT?: Diagnosis of natalizumab-associated PML requires optimised clinical vigilance, reliable and sensitive PCR testing of the JC virus, and broadened criteria for recognition of PML lesions by use of MRI, including contrast enhancement. Optimising the management of IRIS reactions will be needed to improve outcomes. Predictive markers for patients at risk for PML must be sought. It is crucial to monitor the risk incurred during use of natalizumab beyond 3 years.
使用那他珠单抗治疗多发性硬化症会出现罕见的进行性多灶性白质脑病(PML)。2006 年 7 月至 2009 年 11 月,接受那他珠单抗治疗的多发性硬化症患者中有 28 例确诊为 PML。对这些临床病例的评估将有助于为未来的治疗决策提供信息,并改善患者的预后。
在治疗的前 3 年内,接触那他珠单抗的时间越长,发生 PML 的风险就越高。在那他珠单抗上市的前两年没有新病例发生,但截至 2009 年 11 月底,已确诊 28 例,其中 8 例死亡。症状出现的中位治疗持续时间为 25 个月(6-80 个月)。最常见的首发症状包括认知、性格和运动功能的改变,但也有几例患者以癫痫发作作为首发临床事件。尽管 PML 已在未使用任何多发性硬化症治疗药物的患者中发生,但先前使用免疫抑制剂治疗可能会增加风险。除 1 例外,所有患者均通过 MRI 诊断和 CSF 中 JC 病毒检测来确诊。PML 的常规治疗方法是使用血浆置换(PLEX)或免疫吸附来加速那他珠单抗的清除,并缩短那他珠单抗仍处于活跃状态的时间(通常为几个月)。PLEX 后数天至数周内,MRI 上的症状加重和病变增大,提示免疫重建炎症综合征(IRIS)。与 HIV 相关的 PML 相比,这种综合征在那他珠单抗相关 PML 患者中似乎更为常见且更为严重。下一步该怎么做?那他珠单抗相关 PML 的诊断需要优化临床监测、使用可靠和敏感的 PCR 检测 JC 病毒,并扩大 MRI 对 PML 病变的识别标准,包括对比增强。需要优化 IRIS 反应的管理,以改善预后。需要寻找具有 PML 风险的患者的预测标志物。监测使用那他珠单抗 3 年后的风险至关重要。
Zotero 插件