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寡克隆带在多发性硬化症诊断标准中的价值。

The value of oligoclonal bands in the multiple sclerosis diagnostic criteria.

机构信息

Servei de Neurologia-Neuroimmunologia, Centre d'Esclerosi Múltiple de Catalunya (Cemcat), Vall d'Hebron Institut de Recerca, Hospital Universitari Vall d'Hebron, Universitat Autònoma de Barcelona, Barcelona, Spain.

Section of Neuroradiology and Magnetic Resonance Unit, Department of Radiology (IDI), Vall d'Hebron Institut de Recerca, Hospital Universitari Vall d'Hebron, Universitat Autònoma de Barcelona, Barcelona, Spain.

出版信息

Brain. 2018 Apr 1;141(4):1075-1084. doi: 10.1093/brain/awy006.

Abstract

The presence of oligoclonal bands in clinically isolated syndromes is an independent risk factor for developing multiple sclerosis and has been largely excluded from the more recent multiple sclerosis diagnostic criteria. Therefore, our objective was to explore the value of oligoclonal bands in the context of the 2010 McDonald criteria, especially in patients fulfilling exclusively dissemination in space at baseline. For this purpose, we selected 566 patients from a clinically isolated syndrome inception cohort who had IgG oligoclonal bands determination and sufficient data on baseline brain MRI to assess dissemination in space and time. We excluded the cases already fulfilling both dissemination in space and time and divided the remaining 398 into 'no dissemination in space and time' (n = 218), 'dissemination in space' (n = 164) and 'dissemination in time' (n = 16). We assessed Cox proportional hazards regression models with 2010 McDonald as the outcome, using 'no dissemination in space and time' with 0 lesions and negative oligoclonal bands as the reference for different subgroups according to oligoclonal bands status (positive/negative). To assess the diagnostic properties, we selected cases with a follow-up ≥3 years or fulfilling 2010 McDonald within 3 years of the clinically isolated syndrome (n = 314), and compared the performance of all 'dissemination in space' cases (n = 137) versus patients with 'dissemination in space' and positive oligoclonal bands (n = 101). The remaining patients classified as fulfilling 'dissemination in time' or 'no dissemination in space and time' were taken into account to calculate the diagnostic properties. The respective adjusted hazard ratios (95% confidence interval) were 1.5 (0.4-5.7) for 'no dissemination in space and time' with 0 lesions and positive oligoclonal bands, 3.1 (1.4-7.2) for 'no dissemination in space and time' with ≥1 lesions and negative oligoclonal bands, 7.4 (3.5-15.7) for 'no dissemination in space and time' with ≥1 lesions and positive oligoclonal bands, 10.4 (4.8-22.6) for 'dissemination in space' with negative oligoclonal bands, 15.3 (7.5-31.3) for 'dissemination in space' with positive oligoclonal bands, and 9.1 (3.5-23.4) for 'dissemination in time' (not subdivided due to the sample size). The specificity for all cases with 'dissemination in space' was 80.6 and increased to 88.1 after selecting those with positive oligoclonal bands. According to these results, we propose radiological dissemination in space at any time plus positive oligoclonal bands as an additional criterion for diagnosing multiple sclerosis.

摘要

在临床上孤立的综合征中,寡克隆带的存在是发展为多发性硬化症的独立危险因素,并且在最近的多发性硬化症诊断标准中已基本排除在外。因此,我们的目的是探讨寡克隆带在 2010 年 McDonald 标准中的价值,特别是在基线时仅符合空间弥散的患者中。为此,我们从一个临床上孤立的综合征发病队列中选择了 566 例患者,这些患者进行了 IgG 寡克隆带测定,并具有足够的基线脑 MRI 数据来评估空间和时间上的弥散。我们排除了已经同时符合空间和时间弥散的病例,并将其余 398 例分为“无空间和时间弥散”(n=218)、“空间弥散”(n=164)和“时间弥散”(n=16)。我们使用 2010 年 McDonald 作为结果,评估了 Cox 比例风险回归模型,并根据寡克隆带状态(阳性/阴性),将“无空间和时间弥散”且无病变和阴性寡克隆带作为参考,为不同亚组(阳性/阴性)评估不同的亚组。为了评估诊断特性,我们选择了随访时间≥3 年或在临床上孤立的综合征后 3 年内符合 2010 年 McDonald 标准的病例(n=314),并比较了所有“空间弥散”病例(n=137)与“空间弥散”和阳性寡克隆带(n=101)患者的表现。将其余分类为“时间弥散”或“无空间和时间弥散”的患者纳入计算诊断特性。相应的调整后的危险比(95%置信区间)分别为“无空间和时间弥散”且无病变和阳性寡克隆带为 1.5(0.4-5.7),“无空间和时间弥散”且有≥1 个病变和阴性寡克隆带为 3.1(1.4-7.2),“无空间和时间弥散”且有≥1 个病变和阳性寡克隆带为 7.4(3.5-15.7),“空间弥散”且阴性寡克隆带为 10.4(4.8-22.6),“空间弥散”且阳性寡克隆带为 15.3(7.5-31.3),“时间弥散”为 9.1(3.5-23.4)(由于样本量较小,未进行细分)。所有“空间弥散”病例的特异性为 80.6%,选择阳性寡克隆带后增加到 88.1%。根据这些结果,我们提出在任何时候的空间弥散加上阳性寡克隆带作为诊断多发性硬化症的附加标准。

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