首页> 美国卫生研究院文献>The Journal of Neurology and Psychopathology >Spinal cord atrophy and disability in multiple sclerosis over four years: application of a reproducible automated technique in monitoring disease progression in a cohort of the interferon ß-1a (Rebif) treatment trial
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Spinal cord atrophy and disability in multiple sclerosis over four years: application of a reproducible automated technique in monitoring disease progression in a cohort of the interferon ß-1a (Rebif) treatment trial

机译:四年多发性硬化中的脊髓萎缩和残疾:可重复使用的自动化技术在ß-1a干扰素(Rebif)治疗试验队列中监测疾病进展的应用

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摘要

>Background: Pathology in the cervical spinal cord is considered an important cause of disability in multiple sclerosis. However, the majority of serial studies have failed to find a correlation between spinal cord atrophy and disability. >Objectives: To use a highly reproducible and accurate method to quantify spinal cord area change on three dimensional magnetic resonance imaging and relate this to disability change in patients with multiple sclerosis. >Methods: 38 patients with multiple sclerosis (20 with the relapsing–remitting (RRMS) form and 18 with the secondary progressive (SPMS) form) were imaged at baseline and at months 6, 12, 18, and 48 during two treatment trials of the high dose subcutaneous thrice weekly interferon ß-1a (IFNß, Rebif). Thirty one healthy subjects were also imaged at baseline. Upper cervical cord area (UCCA) was measured using Sobel edge detection. >Results: The intraobserver coefficient of variation of the method was 0.42%. A significant reduction in UCCA was detected at month 6 in the placebo group (p = 0.04) and at month 12 for INFß (p = 0.03). The mean reduction of UCCA at month 48 was 5.7% for patients initially on placebo who received treatment at 24 months (RRMS) or at 36 months (SPMS), and 4.5% for those on IFNß throughout the study (p = 0.35). The change in UCCA was significantly correlated with change in the expanded disability status scale at month 12 (r = 0.4, p = 0.016), month 18 (r = 0.32, p = 0.05), and month 48 (r = 0.4, p = 0.016) in the total cohort. >Conclusions: Despite the small number of patients studied and the possible confounding effects of interferon treatment, this study showed that edge detection is reproducible and sensitive to changes in spinal cord area, and that this change is related to changes in clinical disability. This suggests a role for measurement of spinal cord atrophy in monitoring disease progression and possible treatment effects in clinical trails.
机译:>背景:颈脊髓病理被认为是多发性硬化症致残的重要原因。然而,大多数系列研究未能发现脊髓萎缩与残疾之间的相关性。 >目标:要使用高度可重复且准确的方法对三维磁共振成像中的脊髓区域变化进行量化,并将其与多发性硬化症患者的残疾变化相关联。 >方法:在基线以及第6、12、18和8个月对38例多发性硬化症患者(其中20例为复发缓解型(RRMS)形式,18例为继发进行性(SPMS)形式)成像。在两次高剂量皮下每周一次干扰素ß-1a(IFNß,Rebif)的治疗试验中,有48例。在基线还对三十一名健康受试者进行了成像。使用Sobel边缘检测仪测量上颈索面积(UCCA)。 >结果:该方法的观察者内部变异系数为0.42%。安慰剂组在第6个月时检测到UCCA显着降低(p = 0.04),INFß在第12个月时检测到UCCA(p = 0.03)。在整个研究中,最初接受安慰剂的在24个月(RRMS)或在36个月(SPMS)接受治疗的患者在48个月时UCCA的平均减少为5.7%,而在IFNß上接受治疗的患者则为4.5%(p = 0.35)。 UCCA的变化与第12个月(r = 0.4,p = 0.016),第18个月(r = 0.32,p = 0.05)和第48个月(r = 0.4,p =总队列中的0.016)。 >结论:尽管研究的患者人数很少,并且干扰素治疗可能产生混杂效应,但这项研究表明边缘检测可重现并且对脊髓区域的变化敏感,并且这种变化与变化有关在临床残疾中。这暗示了测量脊髓萎缩在监测疾病进展和临床试验中可能的治疗效果中的作用。

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