CORe, Department of Medicine, University of Melbourne, Melbourne, VIC, Australia; Neuroimmunology Centre, Department of Neurology, Royal Melbourne Hospital, Melbourne, VIC, Australia.
Centro SM Dipartimento di Scienze Mediche di Base, Neuroscienze ed Organi di Senso Universita' di Bari, Bari, Italy.
Lancet Child Adolesc Health. 2024 May;8(5):348-357. doi: 10.1016/S2352-4642(24)00047-6. Epub 2024 Mar 25.
High-efficacy disease-modifying therapies have been proven to slow disability accrual in adults with relapsing-remitting multiple sclerosis. However, their impact on disability worsening in paediatric-onset multiple sclerosis, particularly during the early phases, is not well understood. We evaluated how high-efficacy therapies influence transitions across five disability states, ranging from minimal disability to gait impairment and secondary progressive multiple sclerosis, in people with paediatric-onset multiple sclerosis.
Longitudinal data were obtained from the international MSBase registry, containing data from people with multiple sclerosis from 151 centres across 41 countries, and the Italian Multiple Sclerosis and Related Disorders Register, containing data from people with multiple sclerosis from 178 Italian multiple sclerosis centres. People younger than 18 years at the onset of multiple sclerosis symptoms were included, provided they had a confirmed diagnosis of relapsing-remitting multiple sclerosis and at least four Expanded Disability Status Scale (EDSS) scores recorded within 12-month intervals. The primary outcome was the time to change in disability state: minimal disability (EDSS scores 0, 1·0, and 1·5), mild disability (EDSS scores 2·0 and 2·5), moderate disability (EDSS scores 3·0 and 3·5), gait impairment (EDSS scores ≥4·0), and clinician diagnosed secondary progressive multiple sclerosis. A multi-state model was constructed to simulate the natural course of multiple sclerosis, modelling the probabilities of both disability worsening and improvement simultaneously. The impact of high-efficacy disease-modifying therapies (alemtuzumab, cladribine, daclizumab, fingolimod, mitoxantrone, natalizumab, ocrelizumab, rituximab, or autologous haematopoietic stem cell transplantation) and low-efficacy disease-modifying therapies (dimethyl fumarate, glatiramer acetate, interferon beta, or teriflunomide), compared with no treatment, on the course of disability was assessed. Apart from recruitment, individuals with lived experience of multiple sclerosis were not involved in the design and conduct of this study.
A total of 5224 people (3686 [70·6%] female and 1538 [29·4%] male) with mean age at onset of multiple sclerosis 15·24 years (SD 2·52) were included. High-efficacy therapies reduced the hazard of disability worsening across the disability states. The largest reduction (hazard ratio 0·41 [95% CI 0·31-0·53]) was observed in participants who were treated with high-efficacy therapies while in the minimal disability state, compared with those remained untreated. The benefit of high-efficacy therapies declined with increasing disability. Young people with minimal disability who received low-efficacy therapy also experienced a reduced hazard (hazard ratio 0·65 [95% CI 0·54-0·77]) of transitioning to mild disability, in contrast to those who remained untreated.
Treatment of paediatric-onset relapsing-remitting multiple sclerosis with high-efficacy therapy substantially reduces the risk of reaching key disability milestones. This reduction in risk is most pronounced among young people with minimal or mild disability when treatment began. Children with relapsing-remitting multiple sclerosis should be treated early with high-efficacy therapy, before developing significant neurological impairments, to better preserve their neurological capacity.
National Health and Medical Research Council, Australia; MSBase Foundation Fellowship; MS Australia Postdoctoral Fellowship.
已证实高效疾病修正疗法可减缓复发性多发性硬化症成人的残疾累积。然而,其对儿科发病多发性硬化症残疾恶化的影响,特别是在早期阶段,尚不清楚。我们评估了高效疗法如何影响从最小残疾到步态障碍和继发性进行性多发性硬化症等五种残疾状态的转变,对象为儿科发病多发性硬化症患者。
从国际 MSBase 注册中心获得纵向数据,该中心包含来自 41 个国家的 151 个中心的多发性硬化症患者的数据,以及意大利多发性硬化症和相关疾病登记处的数据,该登记处包含来自意大利 178 个多发性硬化症中心的多发性硬化症患者的数据。发病时年龄小于 18 岁的患者纳入研究,前提是他们被确诊为复发性多发性硬化症,并且在 12 个月的间隔内至少有 4 次扩展残疾状态量表(EDSS)评分记录。主要结局是残疾状态变化的时间:最小残疾(EDSS 评分 0、1.0 和 1.5)、轻度残疾(EDSS 评分 2.0 和 2.5)、中度残疾(EDSS 评分 3.0 和 3.5)、步态障碍(EDSS 评分≥4.0)和临床诊断的继发性进行性多发性硬化症。构建了一个多状态模型来模拟多发性硬化症的自然病程,同时对残疾恶化和改善的概率进行建模。评估高效疾病修正疗法(阿仑单抗、克拉屈滨、达利珠单抗、芬戈莫德、米托蒽醌、那他珠单抗、奥瑞珠单抗、利妥昔单抗或自体造血干细胞移植)和低效能疾病修正疗法(二甲法尼酯、聚乙二醇干扰素β-1a、干扰素β或特立氟胺)与不治疗相比,对残疾病程的影响。除招募外,多发性硬化症患者个体没有参与本研究的设计和实施。
共纳入 5224 人(3686 名[70.6%]女性和 1538 名[29.4%]男性),多发性硬化症发病年龄平均为 15.24 岁(标准差 2.52)。高效疗法降低了残疾状态之间残疾恶化的风险。在最小残疾状态下接受高效疗法的参与者的风险降低最大(风险比 0.41[95%CI 0.31-0.53]),与未接受治疗的参与者相比。随着残疾程度的增加,高效疗法的益处下降。接受低效能疗法的最小残疾年轻人也降低了向轻度残疾转变的风险(风险比 0.65[95%CI 0.54-0.77]),与未接受治疗的患者相比。
儿科发病复发性多发性硬化症的高效治疗显著降低了达到关键残疾里程碑的风险。这种风险的降低在最小或轻度残疾的年轻人中最为明显,此时开始治疗。患有复发性多发性硬化症的儿童应在出现明显神经损伤之前尽早接受高效治疗,以更好地保护其神经功能。
澳大利亚国家健康与医学研究委员会;MSBase 基金会奖学金;MS 澳大利亚博士后奖学金。
