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利妥昔单抗降级治疗视神经脊髓炎谱系疾病患者。

Rituximab De-escalation in Patients With Neuromyelitis Optica Spectrum Disorder.

机构信息

From the Department of Neurology (S.D., N.C., J.D.S.); Clinical Investigation Center (N.C., J.D.S.), Strasbourg University Hospital; Department of Neurology (B.A.), APHM, Hôpital de la Timone, Pôle de Neurosciences Cliniques, Marseille; Department of Neurology (X.A.), Montpellier University Hospital; Department of Neurology (B.B.), Rouen University Hospital; Department of Neurology CRC-SEP (J.C.), CHU Toulouse; Department of Neurology, CHU Poitiers (J.C.); Department of Neurology (M.C.), CHU de Nice, UR2CA-URRIS, Nice Côte d'Azur University; Department of Neurology (R.D.), Hôpital Fondation Adolphe de Rothschild, Paris; Department of Neurology (F.D.U.R.A.N.D.-D.U.B.I.E.F.), Sclérose en Plaques, Pathologies de la Myéline et Neuro-inflammation, Hôpital Neurologique, Hospices Civils de Lyon; Department of Neurology (E.M., C.P.), AP-HP, Pitié-Salpêtrière Hospital, Paris; Department of Neurology (Groupe Hospitalier Pellegrin) (A.R.), Centre Hospitalier Universitaire de Bordeaux; Université de Bordeaux (A.R.), INSERM U1215, Neurocentre Magendie; Department of Neurology (H.Z.), University Hospital of Lille, UFR3S Univ-Lille, Inserm U 1172; Service de Neurologie, Sclérose en Plaques, Pathologies de la Myéline et Neuro Inflammation (R.M.), and Centre de Référence des Maladies Inflammatoires Rares du Cerveau et de la Moelle (MIRCEM), Hôpital Neurologique Pierre Wertheimer, Bron; Centre des Neurosciences de Lyon-FORGETTING Team (R.M.), INSERM 1028 and CNRS UMR5292; and Université Claude Bernard Lyon 1 (R.M.), France.

出版信息

Neurology. 2023 Jul 25;101(4):e438-e450. doi: 10.1212/WNL.0000000000207443. Epub 2023 Jun 8.

DOI:10.1212/WNL.0000000000207443
PMID:37290967
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10435052/
Abstract

BACKGROUND AND OBJECTIVES

Exit strategies such as de-escalations have not been evaluated for rituximab in patients with neuromyelitis optica spectrum disorder (NMOSD). We hypothesized that they are associated with disease reactivations and aimed to estimate this risk.

METHODS

We describe a case series of real-world de-escalations from the French NMOSD registry (NOMADMUS). All patients met the 2015 International Panel for NMO Diagnosis (IPND) diagnostic criteria for NMOSD. A computerized screening of the registry extracted patients with rituximab de-escalations and at least 12 months of subsequent follow-up. We searched for 7 de-escalation regimens: scheduled discontinuations or switches to an oral treatment after single infusion cycles, scheduled discontinuations or switches to an oral treatment after periodic infusions, de-escalations before pregnancies, de-escalations after tolerance issues, and increased infusion intervals. Rituximab discontinuations motivated by inefficacy or for unknown purposes were excluded. The primary outcome was the absolute risk of NMOSD reactivation (one or more relapses) at 12 months. AQP4+ and AQP4- serotypes were analyzed separately.

RESULTS

We identified 137 rituximab de-escalations between 2006 and 2019 that corresponded to a predefined group: 13 discontinuations after a single infusion cycle, 6 switches to an oral treatment after a single infusion cycle, 9 discontinuations after periodic infusions, 5 switches to an oral treatment after periodic infusions, 4 de-escalations before pregnancies, 9 de-escalations after tolerance issues, and 91 increased infusion intervals. No group remained relapse-free over the whole de-escalation follow-up (mean: 3.2 years; range: 0.79-9.5), except pregnancies in AQP+ patients. In all groups combined and within 12 months, reactivations occurred after 11/119 de-escalations in patients with AQP4+ NMOSD (9.2%, 95% CI [4.7-15.9]), from 0.69 to 10.0 months, and in 5/18 de-escalations in patients with AQP4- NMOSD (27.8%, 95% CI [9.7-53.5]), from 1.1 to 9.9 months.

DISCUSSION

There is a risk of NMOSD reactivation whatever the rituximab de-escalation regimen.

TRIAL REGISTRATION INFORMATION

Registered on ClinicalTrials.gov: NCT02850705.

CLASSIFICATION OF EVIDENCE

This study provides Class IV evidence that de-escalation of rituximab increases the probability of disease reactivation.

摘要

背景和目的

在视神经脊髓炎谱系疾病(NMOSD)患者中,尚未评估利妥昔单抗的退出策略,如降级治疗。我们假设它们与疾病复发有关,并旨在估计这种风险。

方法

我们描述了法国 NMOSD 登记处(NOMADMUS)的一系列真实世界降级病例。所有患者均符合 2015 年国际 NMOSD 诊断小组(IPND)NMOSD 的诊断标准。该登记处的计算机筛查提取了利妥昔单抗降级治疗且随后至少有 12 个月随访的患者。我们搜索了 7 种降级方案:单次输注周期后定期停药或转换为口服治疗、定期输注后定期停药或转换为口服治疗、妊娠前降级、耐受问题后降级以及增加输注间隔。因无效或其他原因而停止利妥昔单抗治疗的病例被排除在外。主要结局是 12 个月时 NMOSD 复发(一次或多次复发)的绝对风险。AQP4+和 AQP4-血清型分别进行了分析。

结果

我们在 2006 年至 2019 年期间确定了 137 例利妥昔单抗降级治疗,这些治疗对应于一个预先确定的组:单次输注后 13 例停药,单次输注后 6 例转换为口服治疗,周期性输注后 9 例停药,周期性输注后 5 例转换为口服治疗,4 例妊娠前降级,9 例耐受问题后降级,91 例增加输注间隔。除 AQP+患者的妊娠外,整个降级随访期间(平均:3.2 年;范围:0.79-9.5),没有一个组保持无复发。在所有组中,在 12 个月内,AQP4+ NMOSD 患者中有 11/119 例(9.2%,95%CI[4.7-15.9])在 11 次降级治疗后发生了复发,复发时间为 0.69-10.0 个月,而在 AQP4- NMOSD 患者中有 5/18 例(27.8%,95%CI[9.7-53.5])在 5 次降级治疗后发生了复发,复发时间为 1.1-9.9 个月。

讨论

无论利妥昔单抗降级方案如何,都有 NMOSD 复发的风险。

试验注册信息

在 ClinicalTrials.gov 上注册:NCT02850705。

证据分类

这项研究提供了 IV 级证据,表明利妥昔单抗的降级增加了疾病复发的可能性。

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