Clinical trajectories of patients with multiple sclerosis from onset and their relationship with serum neurofilament light chain levels.

IF 2.7 3区 医学 Q2 CLINICAL NEUROLOGY Frontiers in Neurology Pub Date : 2024-10-30 eCollection Date: 2024-01-01 DOI:10.3389/fneur.2024.1477335
Carlos Quintanilla-Bordás, Laura Cubas-Núñez, Jéssica Castillo-Villalba, Sara Carratalá-Boscá, Raquel Gasque-Rubio, Jordi Tortosa-Carreres, Carmen Alcalá, Lorena Forés-Toribio, Celia Lucas, David Gorriz, Francisco Pérez-Miralles, Bonaventura Casanova
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Abstract

Background: Serum neurofilament light chain (sNfL) is a biomarker of neuroaxonal destruction that correlates with acute inflammation (AI) in multiple sclerosis (MS). However, in the treatment era, progression without AI is the main driver of long-term disability. sNfL may provide added value in detecting ongoing axonal damage and neurological worsening in patients without AI. We conducted a prospective three-year study on patients with a first MS relapse to evaluate the basal cut-off value predicting early increased disability unrelated to relapses.

Methods: sNfL levels and AI presence were measured every 6 months during the first year and the Expanded Disability Status Scale (EDSS) was monitored until the third year. Baseline cohorts were stratified by sNfL levels, using a cut-off derived from patients without AI (absence of clinical relapses, new/enlarging T2 lesions, or gadolinium enhancement in magnetic resonance imaging) at year one.

Results: Fifty-one patients were included. A sNfL cut-off of 11 pg/mL predicted sustained neurological worsening independent of AI. Patients exceeding this threshold exhibited features of highly active MS (higher proportion of AI, oligoclonal M bands and higher EDSS). Despite AI ablation, sNfL levels persisted elevated and were significantly associated with increased EDSS at baseline and year 3. Patients with low sNfL and concurrent AI (n = 8) experienced relapses in the optic nerve, brainstem, and spinal cord topographies.

Conclusion: sNfL elevation may detect patients with increased disability even when AI is controlled. This may reveal mechanisms associated with early axonal degeneration and help identify patients at higher risk of progression.

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多发性硬化症患者从发病开始的临床轨迹及其与血清神经丝轻链水平的关系。
背景:血清神经丝蛋白轻链(sNfL)是神经轴突破坏的生物标志物,与多发性硬化症(MS)的急性炎症(AI)相关。然而,在治疗时代,无急性炎症(AI)的病情进展是导致长期残疾的主要原因。sNfL 在检测无急性炎症(AI)患者的轴索持续损伤和神经功能恶化方面可能具有附加价值。我们对首次复发的多发性硬化症患者进行了一项为期三年的前瞻性研究,以评估预测与复发无关的早期残疾增加的基线截断值。根据 sNfL 水平对基线队列进行分层,以第一年无 AI 患者(无临床复发、新的/增大的 T2 病灶或磁共振成像中的钆增强)为分界线:结果:共纳入 51 名患者。sNfL 的临界值为 11 pg/mL,这预示着神经功能持续恶化与 AI 无关。超过这一临界值的患者表现出高度活动性多发性硬化症的特征(更高比例的AI、寡克隆M带和更高的EDSS)。尽管进行了 AI 消融,但 sNfL 水平仍持续升高,并与基线和第 3 年 EDSS 的增加显著相关。sNfL 低且同时患有 AI 的患者(n = 8)在视神经、脑干和脊髓地形图上出现复发。这可能揭示了与早期轴索变性相关的机制,并有助于识别病情恶化风险较高的患者。
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来源期刊
Frontiers in Neurology
Frontiers in Neurology CLINICAL NEUROLOGYNEUROSCIENCES -NEUROSCIENCES
CiteScore
4.90
自引率
8.80%
发文量
2792
审稿时长
14 weeks
期刊介绍: The section Stroke aims to quickly and accurately publish important experimental, translational and clinical studies, and reviews that contribute to the knowledge of stroke, its causes, manifestations, diagnosis, and management.
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