Disease Progression in Multiple System Atrophy: The Value of Clinical Cohorts with Long Follow-Up

IF 7.4 1区 医学 Q1 CLINICAL NEUROLOGY
Tiphaine Saulnier MS, Margherita Fabbri MD, PhD, Anne Pavy-Le Traon MD, PhD, Mélanie Le Goff MS, Catherine Helmer PhD, Patrice Péran PhD, Wassilios G. Meissner MD, PhD, Olivier Rascol MD, PhD, Alexandra Foubert-Samier MD, PhD, Cécile Proust-Lima PhD
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引用次数: 0

Abstract

In their recent publication, Kühnel et al1 described the progression of multiple system atrophy (MSA) in the European MSA study group (EMSA-SG) cohort via an innovative disease progression model (DPM). DPMs are valuable longitudinal methods to describe MSA natural history while accounting for data uncertainty (delayed diagnosis, uncertain timing, heterogeneous staging).2 The mean trajectories of clinical progression are described along the homogeneous disease continuum (Fig. 1C) rather than the observed time since diagnosis (Fig. 1A) thanks to a temporal recalibration of progression according to an individual latent disease time, anchored to MSA disease stage at inclusion.

The population characteristics and the length of individual follow-up are critical in natural history studies and DPMs. Kühnel's study relied on 121 patients with rather advanced stage, outdated diagnosis criteria, and short follow-up of 2 years.1, 3 We replicated Kühnel's analysis on repeated Unified MSA Rating Scale sum scores I (activities of daily living) and II (motor examination) from the French MSA cohort4 (663 patients) with maximum follow-up of 11 years, consensus diagnosis criteria,5 and early stages at entry (see Supplementary Material Data S1 for details). MSA progression spanned a larger period than in the original paper (Fig. 1C) with mean time gaps at inclusion estimated at 3.6 and 9.1 years for moderately-dependent and helpless patients at inclusion, respectively (Fig. 1B right panels); and significant inter-patient differences (SD = 2.14 years). When restricting the sample to 2.5-year follow-up, these differences were smaller, especially among the most aggressively affected patients at entry, with estimates of 2.5 and 6.6 years (Fig. 1B left panels) and smaller inter-patient differences (SD = 0.79 years). This suggests that studies restricted to short-term follow-up overestimate the progression rate and underestimate inter-patient differences.

When applying DPMs, differences across stages should be carefully interpreted. They do not quantify the expected amount of time spent in each stage by a patient, but the time gap between patients entering the study at different stages. Estimating the duration spent in each disability stage requires specific modeling of disability over time.

T.S.: 1A, 1B, 1C, 2A, 2B, 3A

M.F.: 2C, 3B

A.P.L.: 2C, 3B

M.L.: 2C, 3B

C.H.: 2C, 3B

P.P.: 2C, 3B

W.G.M.: 2C, 3B

O.R.: 2C, 3B

A.F.S.: 1A, 1B, 2A, 2C, 3A

C.P.L.: 1A, 1B, 2A, 2C, 3A

多系统萎缩的疾病进展:长期随访的临床队列的价值
在他们最近发表的文章中,k hnel等人1通过一种创新的疾病进展模型(DPM)描述了欧洲MSA研究组(EMSA-SG)队列中多系统萎缩(MSA)的进展。DPMs是描述MSA自然史的有价值的纵向方法,同时考虑到数据的不确定性(延迟诊断、不确定时间、异质性分期)临床进展的平均轨迹是沿着均匀的疾病连续体描述的(图1C),而不是自诊断以来观察到的时间(图1A),这要归功于根据个体潜伏疾病时间对进展进行的时间重新校准,该时间固定在纳入时的MSA疾病阶段。种群特征和个体随访时间在自然史研究和dpm中至关重要。k hnel的研究依赖于121例晚期患者,诊断标准过时,随访时间短,为2年。1,3我们复制了k hnel对法国MSA队列(663例患者)重复的统一MSA评定量表总分I(日常生活活动)和II(运动检查)的分析,最长随访11年,一致的诊断标准,5和入院时的早期阶段(详细信息参见补充材料数据S1)。与原论文相比,MSA进展的时间跨度更大(图1C),中度依赖和无助患者在纳入时的平均时间间隔分别为3.6年和9.1年(图1B右面板);患者间差异显著(SD = 2.14年)。当将样本限制为2.5年随访时,这些差异较小,特别是在入组时受影响最严重的患者中,估计为2.5年和6.6年(图1B左面板),患者间差异较小(SD = 0.79年)。这表明局限于短期随访的研究高估了进展率,低估了患者间差异。在应用dpm时,应该仔细解释不同阶段的差异。他们没有量化患者在每个阶段花费的预期时间,而是在不同阶段进入研究的患者之间的时间间隔。估计在每个残疾阶段花费的时间需要对残疾进行特定的建模。图:1A, 1B, 1C, 2A, 2B, 3AM.F。[c], [b]。2、3磅。: 2c, 3bc。2、3点。2磅,3磅。: 2, 3。: 2℃,3℃。: 1a, 1b, 2a, 2c, 3ac。: 1a, 1b, 2a, 2c, 3a
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来源期刊
Movement Disorders
Movement Disorders 医学-临床神经学
CiteScore
13.30
自引率
8.10%
发文量
371
审稿时长
12 months
期刊介绍: Movement Disorders publishes a variety of content types including Reviews, Viewpoints, Full Length Articles, Historical Reports, Brief Reports, and Letters. The journal considers original manuscripts on topics related to the diagnosis, therapeutics, pharmacology, biochemistry, physiology, etiology, genetics, and epidemiology of movement disorders. Appropriate topics include Parkinsonism, Chorea, Tremors, Dystonia, Myoclonus, Tics, Tardive Dyskinesia, Spasticity, and Ataxia.
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