Background:Today, no specific test for the diagnosis of multiple sclerosis (MS) is available due to the lack of characteristic symptoms at beginning. This circumstance also complicates estimation of disease progression. Recent findings provided evidence for early, non-lesional cerebellar damage in patients with (clinically definite) relapsing-remitting MS. Objective:To investigate if microstructural cerebellar alterations can also serve as early structural biomarker for disease progression and conversion from clinically isolated syndrome (CIS) to MS. Methods:46 patients diagnosed with CIS and 26 age-matched healthy controls were admitted to high-resolution MRI including diffusion tensor imaging (DTI) to examine atrophy and microstructural integrity of the cerebellum. Microstructural integrity of cerebellar white matter was assessed by fractional anisotropy (FA) as derived from DTI. Results:Although all 46 patients of our CIS cohort showed no cerebellar lesions in structural MRI (T1w, T2w, FLAIR), their mean cerebellar FA was already reduced compared to healthy controls. Significant FA reduction at follow-up DTI 6 months after baseline examination was observed. In 16 patients that converted to MS, we found a correlation between initial cerebellar FA and conversion latency (R = 0.71, p < 0.002). Initial cerebellar FA under FAcrit = 0.352 predicted conversion into relapsing-remitting MS within 24 months (FAcrit: mean cerebellar FA of patients with early MS, determined in another study). Conclusion:DTI seems to reflect early tissue injury in beginning MS, when atrophy and lesions are not yet detectable. Decreased cerebellar FA in patients with CIS might indicate an active and unstable disease stage, resulting in a shorter conversion time into MS.

译文

背景:由于一开始缺乏特征性症状,目前尚无用于诊断多发性硬化症(MS)的特异性测试。这种情况也使疾病进展的估计复杂化。最新发现为患有(临床上明确的)复发缓解型MS的患者早期,非病变性小脑损伤提供了证据。
目的:探讨微结构小脑改变是否还可以作为疾病发展和从临床孤立综合征(CIS)转变为MS的早期结构生物标志物。
方法:46例确诊为CIS的患者和26例年龄相匹配的健康对照者接受包括弥散张量成像(DTI)在内的高分辨率MRI检查,以检查小脑的萎缩和微结构完整性。小脑白质的微结构完整性通过衍生自DTI的分数各向异性(FA)进行评估。
结果:尽管我们的CIS队列中的所有46例患者在结构MRI(T1w,T2w,FLAIR)中均未显示小脑病变,但与健康对照组相比,他们的平均小脑FA已有所减少。在基线检查后6个月的随访DTI中观察到了显着的FA减少。在16名转化为MS的患者中,我们发现初始小脑FA与转化潜伏期之间存在相关性(R = 0.71,p <0.002)。在FAcrit = 0.352以下的初始小脑FA预计在24个月内会转化为复发缓解型MS(FAcrit:早期MS患者的平均小脑FA,在另一项研究中确定)。
结论:DTI似乎反映了MS早期的组织损伤,当时尚无法检测到萎缩和病变。 CIS患者的小脑FA降低可能表明疾病的活动期和不稳定期,从而缩短了MS的转化时间。

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