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神经影像学标志物在癫痫中的应用:进展及与神经胶质细胞的相关性。

Neuroimaging biomarkers for epilepsy: advances and relevance to glial cells.

机构信息

Department of Pediatrics, School of Medicine, Loma Linda University, Loma Linda, CA, USA; Division of Interdisciplinary Studies, School of Behavioral Health, Loma Linda University, Loma Linda, CA, USA; Cell and Molecular Development and Biology Program, University of California, Riverside, CA, USA; Neuroscience Graduate Program, University of California, Riverside, CA, USA.

出版信息

Neurochem Int. 2013 Dec;63(7):712-8. doi: 10.1016/j.neuint.2013.05.001. Epub 2013 May 9.

Abstract

Glial cells play an important role in normal brain function and emerging evidence would suggest that their dysfunction may be responsible for some epileptic disease states. Neuroimaging of glial cells is desirable, but there are no clear methods to assess neither their function nor localization. Magnetic resonance imaging (MRI) is now part of a standardized epilepsy imaging protocol to assess patients. Structural volumetric and T2-weighted imaging changes can assist in making a positive diagnosis in a majority of patients. The alterations reported in structural and T2 imaging is predominantly thought to reflect early neuronal loss followed by glial hypertrophy. MR spectroscopy for myo-inositol is a being pursued to identify glial alterations along with neuronal markers. Diffusion weighted imaging (DWI) is ideal for acute epileptiform events, but is not sensitive to either glial cells or neuronal long-term changes found in epilepsy. However, DWI variants such as diffusion tensor imaging or q-space imaging may shed additional light on aberrant glial function in the future. The sensitivity and specificity of PET radioligands, including those targeting glial cells (translocator protein) hold promise in being able to image glial cells. As the role of glial function/dysfunction in epilepsy becomes more apparent neuroimaging methods will evolve to assist the clinician and researcher in visualizing their location and function.

摘要

神经胶质细胞在大脑正常功能中起着重要作用,新出现的证据表明,它们的功能障碍可能是导致某些癫痫疾病状态的原因。神经胶质细胞的神经影像学是理想的,但目前还没有明确的方法来评估其功能或定位。磁共振成像(MRI)现在是癫痫成像标准方案的一部分,用于评估患者。结构容积和 T2 加权成像的变化有助于对大多数患者做出阳性诊断。据报道,结构和 T2 成像的改变主要反映了早期神经元丢失,随后是神经胶质细胞肥大。正在研究肌醇的磁共振波谱,以确定神经胶质改变以及神经元标记物。扩散加权成像(DWI)是急性癫痫样事件的理想选择,但对癫痫中发现的神经胶质细胞或神经元的长期变化不敏感。然而,扩散张量成像或 q 空间成像等 DWI 变体可能会在未来为异常神经胶质功能提供更多的线索。包括针对神经胶质细胞(转位蛋白)的正电子发射断层扫描放射性配体的敏感性和特异性在能够对神经胶质细胞进行成像方面具有广阔的前景。随着神经胶质功能/障碍在癫痫中的作用变得更加明显,神经影像学方法将不断发展,以帮助临床医生和研究人员观察它们的位置和功能。

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