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基底节、丘脑和大脑新皮质萎缩可预测多发性硬化认知处理速度减慢。

Basal ganglia, thalamus and neocortical atrophy predicting slowed cognitive processing in multiple sclerosis.

机构信息

Department of Neurology, Coimbra University Hospitals, Coimbra, Portugal.

出版信息

J Neurol. 2012 Jan;259(1):139-46. doi: 10.1007/s00415-011-6147-1. Epub 2011 Jul 1.

DOI:10.1007/s00415-011-6147-1
PMID:21720932
Abstract

Information-processing speed (IPS) slowing is a primary cognitive deficit in multiple sclerosis (MS). Basal ganglia, thalamus and neocortex are thought to have a key role for efficient information-processing, yet the specific relative contribution of these structures for MS-related IPS impairment is poorly understood. To determine if basal ganglia and thalamus atrophy independently contribute to visual and auditory IPS impairment in MS, after controlling for the influence of neocortical volume, we enrolled 86 consecutive MS patients and 25 normal controls undergoing 3T brain MRI and neuropsychological testing. Using Sienax and FIRST software, neocortical and deep gray matter (DGM) volumes were calculated. Neuropsychological testing contributed measures of auditory and visual IPS using the Paced Auditory Serial Addition Test (PASAT) and the Symbol Digit Modalities Test (SDMT), respectively. MS patients exhibited significantly slower IPS relative to controls and showed reduction in neocortex, caudate, putamen, globus pallidus, thalamus and nucleus accumbens volume. SDMT and PASAT were significantly correlated with all DGM regions. These effects were mitigated by controlling for the effects of neocortical volume, but all DGM volumes remained significantly correlated with SDMT, putamen (r = 0.409, p < 0.001) and thalamus (r = 0.362, p < 0.001) having the strongest effects, whereas for PASAT, the correlation was significant for putamen (r = 0.313, p < 0.01) but not for thalamus. We confirm the significant role of thalamus atrophy in MS-related IPS slowing and find that putamen atrophy is also a significant contributor to this disorder. These DGM structures have independent, significant roles, after controlling for the influence of neocortex atrophy.

摘要

信息处理速度(IPS)减慢是多发性硬化症(MS)的主要认知缺陷。基底神经节、丘脑和新皮层被认为对有效信息处理具有关键作用,但这些结构对 MS 相关 IPS 损害的具体相对贡献知之甚少。为了确定基底神经节和丘脑萎缩是否独立导致 MS 患者的视觉和听觉 IPS 损害,在控制新皮层体积的影响后,我们招募了 86 名连续 MS 患者和 25 名正常对照者进行 3T 脑 MRI 和神经心理学测试。使用 Sienax 和 FIRST 软件计算新皮层和深部灰质(DGM)体积。神经心理学测试使用听觉连续加法测试(PASAT)和符号数字模态测试(SDMT)分别贡献 IPS 的听觉和视觉测量值。MS 患者的 IPS 明显慢于对照组,且新皮层、尾状核、壳核、苍白球、丘脑和伏隔核体积减少。SDMT 和 PASAT 与所有 DGM 区域显著相关。通过控制新皮层体积的影响,这些效应得到缓解,但所有 DGM 体积仍然与 SDMT 显著相关,与壳核(r = 0.409,p < 0.001)和丘脑(r = 0.362,p < 0.001)的相关性最强,而对于 PASAT,与壳核的相关性显著(r = 0.313,p < 0.01),但与丘脑无关。我们证实了丘脑萎缩在 MS 相关 IPS 减慢中的重要作用,并发现壳核萎缩也是该疾病的重要原因。这些 DGM 结构在控制新皮层萎缩的影响后具有独立的、显著的作用。

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