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首页> 外文期刊>Neurology: Official Journal of the American Academy of Neurology >The metabolic topography of essential blepharospasm: a focal dystonia with general implications.
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The metabolic topography of essential blepharospasm: a focal dystonia with general implications.

机译:基本的代谢地形与一般睑痉挛:局灶性肌张力障碍的影响。

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摘要

OBJECTIVE: To determine the metabolic topography of essential blepharospasm (EB). BACKGROUND: EB is a cranial dystonia of unknown etiology and anatomic localization. The authors have used 18F-fluorodeoxyglucose (FDG) and PET with network analysis to identify distinctive patterns of regional metabolic abnormality associated with idiopathic torsion dystonia (ITD), as well as sleep induction during PET imaging to suppress involuntary movements, thereby reducing this potential confound in the analysis. METHODS: Six patients with EB and six normal volunteers were scanned with FDG-PET. Scans were performed twice: once in wakefulness and once following sleep induction. The authors used statistical parametric mapping to compare glucose metabolism between patients with EB and control subjects in each condition. They also quantified the expression of the previously identified ITD-related metabolic networks in each subject in both conditions. RESULTS: With active involuntary movements during wakefulness, the EB group exhibited hypermetabolism of the cerebellum and pons. With movement suppression during sleep, the EB group exhibited superior-medial frontal hypometabolism in a region associated with cortical control of eyelid movement. Network analysis demonstrated a specific metabolic covariance pattern associated with ITD was also expressed in the patients with EB in both the sleep and wake conditions. CONCLUSION: These findings suggest that the clinical manifestations of EB are associated with abnormal metabolic activity in the pons and cerebellum, whereas the functional substrate of the disorder may be associated with abnormalities in cortical eyelid control regions. Furthermore, ITD-related networks are expressed in patients with EB, suggesting a functional commonality between both forms of primary dystonia.
机译:目的:确定代谢地形基本睑痉挛(EB)。是一种病因不明的颅肌张力障碍和的解剖定位。18 f-fluorodeoxyglucose (FDG)和宠物与网络分析识别的独特模式区域代谢异常有关特发性扭转肌张力障碍(ITD),以及在PET成像抑制睡眠诱导不随意运动,从而减少在分析潜在的混淆。EB患者和6个正常的志愿者与正子扫描。一旦在清醒和睡眠归纳。参数映射比较葡萄糖代谢EB患者和对照组之间每个条件。先前确定的表情在每个主题ITD-related代谢网络这两个条件。运动中觉醒,EB组小脑代谢亢进和展出脑桥。EB组表现出superior-medial额地区与代谢减退皮质眼睑运动的控制。分析了特定的代谢协方差模式与ITD也有关EB患者中表达的睡眠和清醒的条件。研究结果表明,临床表现海尔哥哥与代谢异常有关活动在脑桥小脑,而功能性衬底的障碍与皮质眼睑异常有关控制区域。网络是EB患者中表达,建议功能之间的共性形式的原发性肌张力障碍。

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