Identification of alemtuzumab-suitable multiple sclerosis patients in Slovakia and sequencing of post-alemtuzumab immunomodulatory treatment.

IF 4.7 2区 医学 Q1 CLINICAL NEUROLOGY
Therapeutic Advances in Neurological Disorders Pub Date : 2024-10-28 eCollection Date: 2024-01-01 DOI:10.1177/17562864241285556
Ema Kantorová, Marianna Vítková, Martina Martiníková, Andrea Cimprichová, Miriam Fedicˇová, Slavomíra Kovácˇová, Miroslav Mako, Juraj Cisár, Viera Hancˇinová, Jarmila Szilasiová, Peter Koleda, Jana RoháIˇová, Jana Polóniová, Martin Karlík, Darina Slezáková, Eleonóra Klímová, Matúš Maciak, Egon Kurcˇa, Petra Hnilicová
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引用次数: 0

Abstract

Background: Alemtuzumab (ALEM) is a humanised monoclonal antibody that depletes circulating lymphocytes by selectively targeting CD52, which is expressed in high levels on T- and B-lymphocytes. This depletion is followed by lymphocyte repopulation and a cytokine expression shift towards a lesser inflammatory profile, both of which may contribute to prolonged efficacy. National recommendations for enrolling and treating multiple sclerosis (MS) patients with ALEM have been established. However, there are no recommendations in place for the treatment of MS reactivation after the ALEM treatment.

Objectives: To evaluate the effectiveness and safety of the use of ALEM and to analyse subsequent disease-modifying treatments (DMTs). A multidimensional prediction model was developed to make a patient-specific prognosis regarding the response to ALEM.

Design: A multicentre, prospective, non-controlled, non-interventional, observational cohort study.

Methods: Relapsing multiple sclerosis patients (RMSp) who received ⩾1 dose of ALEM were enrolled. In each treatment year, the following baseline and prospective data were collected: age, MS history, number, type and duration of previous disease-modifying treatment (PDMT), relapse rate (REL), expanded disability status scale (EDSS), magnetic resonance imaging and serious adverse events (AE). In cases of reactivation of MS, all data about the subsequent DMT were collected.

Results: A total of 142 RMSp from 10 MS Slovak Centres fulfilled the inclusion criteria. The average age was 35 years (standard error 8.56). The overall average EDSS was 3.87 (1.46) when ALEM was started. The average duration of PDMT was 6.0 (4.04) years, and the median number of PDMTs was 3 (0-5), while the patients were mostly treated with 2 or 3 DMTs (>65.00%). Post-ALEM treatment was needed in 39 cases (27.46%). The most frequent post-ALEM treatment indicated was ocrelizumab, followed by natalizumab (NAT), siponimod and cladribine. The ocrelizumab and NAT treatment bring little benefit to patients. Siponimod showed less EDSS increase in contrast to ocrelizumab and NAT. Another repopulation therapy, cladribine, may also be an effective option. Statistically significant predictors for the expected EDSS are age (p-value <0.0001), number of ALEM cycles (0.0066), high number of PDMT (0.0459) and the occurrence of relapses (<0.0001). There was no statistically significant effect on the patient's gender (0.6038), duration of disease-modifying treatment before alemtuzumab (0.4466), or the occurrence of AE (0.6668).

Conclusion: The study confirms the positive effect of ALEM on clinical and radiological outcomes. We need more data from long-term sequencing studies.

确定斯洛伐克适合使用阿仑珠单抗的多发性硬化症患者,并对阿仑珠单抗后的免疫调节治疗进行排序。
研究背景阿来珠单抗(Alemtuzumab,ALEM)是一种人源化单克隆抗体,通过选择性靶向T淋巴细胞和B淋巴细胞高表达的CD52,消耗循环淋巴细胞。耗竭后,淋巴细胞会重新增殖,细胞因子的表达也会向炎症较轻的方向转变,这两点可能有助于延长疗效。目前已制定了关于多发性硬化症(MS)ALEM 患者入组和治疗的国家建议。然而,目前还没有针对 ALEM 治疗后多发性硬化症再激活的治疗建议:目的:评估使用 ALEM 的有效性和安全性,并分析随后的疾病改变疗法(DMT)。开发了一个多维预测模型,以针对患者对ALEM的反应进行预后分析:多中心、前瞻性、非对照、非干预、观察性队列研究:方法:研究对象为接受过一次ALEM治疗的复发性多发性硬化症患者(RMSp)。在每个治疗年度,收集以下基线数据和前瞻性数据:年龄、多发性硬化病史、既往疾病修饰治疗(PDMT)的次数、类型和持续时间、复发率(REL)、残疾状况扩展量表(EDSS)、磁共振成像和严重不良事件(AE)。在多发性硬化症再次复发的病例中,收集了有关后续疾病修饰治疗的所有数据:共有来自斯洛伐克 10 个多发性硬化症中心的 142 名多发性硬化症患者符合纳入标准。平均年龄为 35 岁(标准误差为 8.56)。开始接受 ALEM 治疗时,EDSS 总平均值为 3.87(1.46)。PDMT的平均持续时间为6.0(4.04)年,PDMT的中位数为3(0-5)次,而患者大多接受了2或3次DMT治疗(>65.00%)。39例患者(27.46%)需要接受ALEM后治疗。最常见的ALEM后治疗药物是奥克雷珠单抗,其次是纳他珠单抗(NAT)、西泊尼莫德和克来曲滨。奥克利珠单抗和纳他珠单抗治疗对患者的益处不大。与奥克利珠单抗和纳他珠单抗相比,西泊尼莫德的EDSS增加较少。另一种再植疗法克拉德里滨也可能是一种有效的选择。对预期 EDSS 有统计学意义的预测因素是年龄(P 值 结论):该研究证实了 ALEM 对临床和放射学结果的积极影响。我们需要更多来自长期测序研究的数据。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
8.30
自引率
1.70%
发文量
62
审稿时长
15 weeks
期刊介绍: Therapeutic Advances in Neurological Disorders is a peer-reviewed, open access journal delivering the highest quality articles, reviews, and scholarly comment on pioneering efforts and innovative studies across all areas of neurology. The journal has a strong clinical and pharmacological focus and is aimed at clinicians and researchers in neurology, providing a forum in print and online for publishing the highest quality articles in this area.
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