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Natalizumab Discontinuation and Treatment Strategies in Patients with Multiple Sclerosis (MS): A Retrospective Study from Two Italian MS Centers

机译:多发性硬化症(MS)患者的那他珠单抗停药和治疗策略:来自两个意大利MS中心的回顾性研究

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摘要

Introduction: Natalizumab (NTZ) discontinuation can be followed by multiple sclerosis (MS) disease reactivation. Currently no disease-modifying drug (DMD) has been shown to be able to abolish disease reactivation. The aims of the current study were: (1) to determine the frequency of MS reactivation after NTZ discontinuation; (2) to evaluate predictors of reactivation risk, and (3) to compare the effect of different treatments in reducing this risk. Methods: Data from 132 patients with MS followed-up for 2 years before NTZ treatment and 1 year after interruption were collected from two Italian MS centers and retrospectively evaluated. Results: Overall, 72 of 132 patients (54.5%) had relapses after NTZ discontinuation and 60 of 125 patients (48%), who had magnetic resonance imaging, had radiological reactivation. Rebound was observed in 28 of 132 patients (21.2%). A higher number of relapses in the 2 years before NTZ treatment, a longer washout period, and a lower number NTZ infusions correlated with reactivation and rebound. Untreated patients (n = 37) had higher clinical and radiological activity and rebound in comparison to patients receiving DMDs. Moreover, a lower risk of relapses was found in patients treated with second-line therapies (NTZ and fingolimod) than in those treated with first-line therapies (interferon beta, glatiramer acetate, teriflunomide, azathioprine). Interestingly, no disease reactivation in off-label treatment (rituximab, autologous hematopoietic stem cell transplantation) was observed. Conclusion: NTZ discontinuation is a risk for MS reactivation and rebound. An alternative treatment should be promptly resumed mainly in patients with a previous very active disease course and with a shorter NTZ therapy. Second-line therapies demonstrate superiority in preventing relapses after NTZ discontinuation.
机译:简介:停用那他珠单抗(NTZ)之后可以重新激活多发性硬化症(MS)。目前,尚无改善疾病的药物(DMD)能够消除疾病的活化。当前研究的目的是:(1)确定NTZ停用后MS重新激活的频率; (2)评估重新激活风险的预测因子,以及(3)比较不同疗法降低这种风险的效果。方法:从意大利的两个MS中心收集了132例MS患者的数据,这些患者在NTZ治疗前2年和中断后1年进行了随访。结果:总体上,132例患者中有72例(54.5%)在NTZ停用后复发,而125例中有60例(48%)接受了核磁共振成像,并进行了放射学检查。 132名患者中有28名(21.2%)出现反弹。 NTZ治疗前2年复发次数较多,洗脱时间较长,NTZ输注次数较少与再激活和反弹有关。与接受DMD的患者相比,未经治疗的患者(n = 37)具有更高的临床和放射学活性以及反弹。此外,与一线疗法(干扰素β,醋酸格拉替雷,特立氟胺,硫唑嘌呤)相比,二线疗法(NTZ和芬戈莫德)治疗的患者复发风险更低。有趣的是,在标签外治疗(利妥昔单抗,自体造血干细胞移植)中未观察到疾病再激活。结论:NTZ停药是MS重新激活和反弹的风险。主要在以前有非常活跃的病程和较短的NTZ治疗的患者中应立即恢复替代治疗。二线疗法显示出在NTZ停用后预防复发方面的优势。

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