丘脑损伤与多发性硬化症的长期残疾进展。

Thalamic damage and long-term progression of disability in multiple sclerosis.

机构信息

Neuroimaging Research Unit, Institute of Experimental Neurology, Division of Neuroscience, Scientific Institute and University Hospital San Raffaele, via Olgettina 60, 20132 Milan, Italy.

出版信息

Radiology. 2010 Nov;257(2):463-9. doi: 10.1148/radiol.10100326. Epub 2010 Aug 19.

DOI:10.1148/radiol.10100326

PMID:20724544

Abstract

PURPOSE

To estimate the relative contributions of baseline thalamic atrophy and abnormalities shown at magnetization transfer (MT) magnetic resonance (MR) imaging, as well as their 12-month changes, in predicting accumulation of disability in a relatively large sample of patients with relapse-onset multiple sclerosis (MS) during an 8-year period.

MATERIALS AND METHODS

The study was conducted with approval of the institutional review board. Written informed consent was obtained from each participant. Conventional and MT MR imaging of the brain was performed at baseline and at 12-month follow-up in 13 healthy control subjects and 73 patients with relapse-onset MS; participants were monitored with clinical visits for 8 years. The following parameters were evaluated at baseline and at 12-month follow-up: volume of lesions with high signal intensity at T2-weighted imaging, volume of lesions with low signal intensity at T1-weighted imaging, mean lesion MT ratio, thalamic fraction, and thalamic MT ratio. A multivariate analysis was used to evaluate the predictors of long-term neurologic deterioration.

RESULTS

At 8-year follow-up, 44 patients showed worsening disability. During follow-up, reduction in thalamic fraction was more pronounced in patients with relapsing-remitting MS than in those with secondary progressive MS (P = .001); thalamic MT ratio decreased only in patients with secondary progressive MS (P = .007). In the multivariable model, baseline thalamic fraction (odds ratio = 0.62, P = .01) and mean percentage change in lesion MT ratio after 12 months (odds ratio = 0.90, P = .04) were independent predictors of worsening disability at 8 years. At baseline, thalamic fraction was correlated with lesion volumes at T2-weighted imaging (r = -0.75, P < .001) and T1-weighted imaging (r = -0.60, P < .001).

CONCLUSION

Thalamic atrophy is correlated with long-term accumulation of disability in patients with MS. White matter lesions are likely to contribute to the loss of tissue seen in the thalamus of patients with MS.

摘要

目的

评估基线丘脑萎缩和磁化传递（MT）磁共振（MR）成像显示的异常在预测复发型多发性硬化（MS）患者相对较大样本中残疾累积方面的相对贡献，以及在 8 年期间的 12 个月变化。

材料和方法

该研究获得了机构审查委员会的批准。每位参与者均获得书面知情同意。在 13 名健康对照者和 73 名复发型 MS 患者中，分别在基线和 12 个月随访时进行了常规和 MT 脑 MRI；通过临床随访监测参与者 8 年。在基线和 12 个月随访时评估以下参数：T2 加权成像高信号病变体积、T1 加权成像低信号病变体积、平均病变 MT 比、丘脑分数和丘脑 MT 比。使用多元分析评估长期神经功能恶化的预测因素。

结果

在 8 年随访时，44 名患者出现残疾恶化。在随访期间，缓解-复发型 MS 患者的丘脑分数降低更为明显，而继发进展型 MS 患者则较轻（P =.001）；仅继发进展型 MS 患者的丘脑 MT 比下降（P =.007）。在多变量模型中，基线丘脑分数（优势比 = 0.62，P =.01）和 12 个月后病变 MT 比的平均百分比变化（优势比 = 0.90，P =.04）是 8 年后残疾恶化的独立预测因素。基线时，丘脑分数与 T2 加权成像（r = -0.75，P <.001）和 T1 加权成像（r = -0.60，P <.001）的病变体积相关。