Slowly Expanding Lesions Predict 9-Year Multiple Sclerosis Disease Progression.

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Neurology(R) neuroimmunology & neuroinflammation Pub Date : 2022-02-01 Print Date: 2022-03-01 DOI:10.1212/NXI.0000000000001139

Paolo Preziosa, Elisabetta Pagani, Alessandro Meani, Lucia Moiola, Mariaemma Rodegher, Massimo Filippi, Maria A Rocca

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引用次数: 26

Abstract

Background and objectives: Chronic active lesions contribute to multiple sclerosis (MS) severity, but their association with long-term disease progression has not been evaluated yet. White matter (WM) lesions showing linear expansion over time on serial T₁- and T₂-weighted scans (i.e., slowly expanding lesions [SELs]) have been proposed as a marker of chronic inflammation. In this study, we assessed whether SEL burden and microstructural abnormalities were associated with Expanded Disability Status Scale (EDSS) score worsening and secondary progressive (SP) conversion at 9.1-year follow-up in patients with relapsing-remitting (RR) MS.

Methods: In 52 patients with RRMS, SELs were identified among WM lesions by linearly fitting the Jacobian of the nonlinear deformation field between time points obtained combining 3T brain T₁- and T₂-weighted scans acquired at baseline and months 6, 12, and 24. Logistic regression analysis was applied to investigate the associations of SEL number, volume, magnetization transfer ratio (MTR), and T₁-weighted signal intensity with disability worsening (i.e., EDSS score increase) and SP conversion after a median follow-up of 9.1 years.

Results: At follow-up, 20/52 (38%) patients with MS showed EDSS score worsening; 13/52 (25%) showed SP conversion. A higher baseline EDSS score (for each point higher: OR = 3.15 [95% CI = 1.61; 8.38], p = 0.003), a higher proportion of SELs among baseline lesions (for each % increase: OR = 1.22 [1.04; 1.58], p = 0.04), and lower baseline MTR values of SELs (for each % higher: OR = 0.66 [0.41; 0.92], p = 0.033) were significant independent predictors of EDSS score worsening at follow-up (C-index = 0.892). A higher baseline EDSS score (for each point higher: OR = 6.37 [1.98; 20.53], p = 0.002) and lower baseline MTR values of SELs (for each % higher: OR = 0.48 [0.25; 0.89], p = 0.02) independently predicted SPMS conversion (C-index = 0.947).

Discussion: The proportion of SELs is associated with MS progression after 9 years. More severe SEL microstructural abnormalities independently predict EDSS score worsening and SPMS conversion. The quantification of SEL burden and damage using T₁-, T₂-weighted, and MTR sequences may identify patients with RRMS at a higher risk of long-term disability progression and SPMS conversion.

Classification of evidence: This study provides Class III evidence that in patients with RRMS starting treatment with natalizumab or fingolimod, the proportion of SELs on brain MRI was associated with EDSS score worsening and SPMS conversion at 9-year follow-up.

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缓慢扩大的病变预测9年多发性硬化症的进展。

背景和目的:慢性活动性病变有助于多发性硬化症(MS)的严重程度，但其与长期疾病进展的关系尚未得到评估。在连续T1和t2加权扫描中，白质(WM)病变随时间呈线性扩张(即缓慢扩张的病变[SELs])被认为是慢性炎症的标志。在这项研究中，我们评估了SEL负担和显微结构异常是否与扩展残疾状态量表(EDSS)评分恶化和复发缓解型(RR) ms患者的继发性进展(SP)转换有关。在52例RRMS患者中，通过线性拟合在基线和第6、12和24个月获得的3T脑T1和t2加权扫描所获得的时间点之间的非线性变形场的雅可比矩阵，在WM病变中识别SELs。采用Logistic回归分析研究中位随访9.1年后，SEL数、体积、磁化传递比(MTR)和t1加权信号强度与残疾加重(即EDSS评分升高)和SP转换的关系。结果:随访时，52例MS患者中有20例(38%)出现EDSS评分加重;13/52(25%)发生SP转化。基线EDSS评分较高(每高一分:OR = 3.15 [95% CI = 1.61;8.38]， p = 0.003)， SELs在基线病变中的比例更高(每增加%:OR = 1.22 [1.04;1.58]， p = 0.04)， SELs的基线MTR值较低(每高%:OR = 0.66 [0.41;0.92]， p = 0.033)是随访时EDSS评分恶化的显著独立预测因子(C-index = 0.892)。基线EDSS评分越高(每高一分OR = 6.37 [1.98;20.53]， p = 0.002)和较低的基线MTR值(每高%:OR = 0.48 [0.25;0.89]， p = 0.02)独立预测SPMS转换(C-index = 0.947)。讨论:9年后，SELs的比例与MS进展有关。更严重的SEL显微结构异常独立预测EDSS评分恶化和SPMS转换。使用T1-、t2 -加权和MTR序列量化SEL负担和损伤，可以识别长期残疾进展和SPMS转化风险较高的RRMS患者。证据分类:本研究提供III类证据，在开始接受natalizumab或fingolimod治疗的RRMS患者中，脑MRI上SELs的比例与9年随访时EDSS评分恶化和SPMS转换相关。

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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Neurology(R) neuroimmunology & neuroinflammation

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