Brain Atrophy as an Outcome of Disease-Modifying Therapy for Remitting-Relapsing Multiple Sclerosis.

IF 2.2 Q3 CLINICAL NEUROLOGY
Magdalena Chylińska, Jakub Komendziński, Adam Wyszomirski, Bartosz Karaszewski
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引用次数: 0

Abstract

Introduction: Currently, clinical trials of DMTs strive to determine their effect on neuroinflammation and neurodegeneration. We aimed to determine the impact of currently used DMTs on brain atrophy and disability in RRMS. The main goal of this review is to evaluate the neuroprotective potential of MS therapy and assess its impact on disability.

Methods: We performed a systematic analysis of clinical trials that used brain atrophy as an outcome or performed post hoc analysis of volumetric MRI parameters to assess the neuroprotective potential of applied therapies. Trials between 2008 and 2019 that included published results of brain parenchymal fraction (BPF) change and brain volume loss (BVL) in the period from baseline to week 96 or longer were considered.

Results: Twelve from 146 clinical trials met the inclusion criteria and were incorporated into the analysis. DMTs that presented a large reduction in BVL also exhibited robust effects on clinical disability worsening, e.g., alemtuzumab with a 42% risk reduction in 6-month confirmed disability accumulation (p = 0.0084), ocrelizumab with a 40% risk reduction in 6-month confirmed disability progression (p = 0.003), and other DMTs (cladribine and teriflunomide) with moderate influence on brain atrophy were also associated with a marked impact on disability worsening. Dimethyl fumarate (DEFINE) and fingolimod (FREEDOMS I) initially exhibited significant effect on BVL; however, this effect was not confirmed in further clinical trials: CONFIRM and FREEDOMS II, respectively. Peg-IFN-β1a shows a modest effect on BVL and disability worsening.

Conclusion: Our results show that BVL in one of the components of clinical disability worsening, together with other variables (lesion volume and annualized relapse rate). Standardization of atrophy measurement technique as well as harmonization of disability worsening and progression criteria in further clinical trials are of utmost importance as they enable a reliable comparison of neuroprotective potential of DMTs.

Abstract Image

缓解-复发多发性硬化症疾病改善治疗的结果脑萎缩。
目前,dmt的临床试验努力确定其对神经炎症和神经变性的影响。我们的目的是确定目前使用的dmt对RRMS脑萎缩和残疾的影响。本综述的主要目的是评估多发性硬化症治疗的神经保护潜力和评估其对残疾的影响。方法:我们对以脑萎缩为结果的临床试验进行了系统分析,或对体积MRI参数进行事后分析,以评估应用疗法的神经保护潜力。2008年至2019年期间的试验,包括从基线到第96周或更长时间内脑实质分数(BPF)变化和脑容量损失(BVL)的已发表结果。结果:146项临床试验中有12项符合纳入标准,纳入分析。大幅降低BVL的dmt也对临床残疾恶化表现出强大的影响,例如,阿仑单抗在6个月确认的残疾积累中降低42%的风险(p = 0.0084), ocrelizumab在6个月确认的残疾进展中降低40%的风险(p = 0.003),其他对脑萎缩有中等影响的dmt (cladribine和teriflunomide)也与对残疾恶化的显着影响相关。富马酸二甲酯(DEFINE)和fingolimod (FREEDOMS I)最初对BVL有显著影响;然而,这种效果并没有在进一步的临床试验中得到证实:分别是CONFIRM和FREEDOMS II。Peg-IFN-β1a对BVL和残疾恶化的影响不大。结论:我们的研究结果表明,BVL是临床残疾恶化的一个组成部分,与其他变量(病变体积和年复发率)一起。在进一步的临床试验中,萎缩测量技术的标准化以及残疾恶化和进展标准的统一是至关重要的,因为它们可以可靠地比较dmt的神经保护潜力。
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来源期刊
Multiple Sclerosis International
Multiple Sclerosis International CLINICAL NEUROLOGY-
自引率
0.00%
发文量
6
审稿时长
15 weeks
期刊介绍: Multiple Sclerosis International is a peer-reviewed, Open Access journal that publishes original research articles, review articles, and clinical studies related to all aspects of multiple sclerosis, including clinical neurology, neuroimaging, neuropathology, therapeutics, genetics, neuroimmunology, biomarkers, psychology and neurorehabilitation.
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