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全身性癫痫患者体内苯二氮䓬受体密度改变的体内研究证明

In vivo demonstration of altered benzodiazepine receptor density in patients with generalised epilepsy.

作者信息

Savic I, Pauli S, Thorell J O, Blomqvist G

机构信息

Department of Clinical Neurophysiology, Karolinska Pharmacy, Karolinska Hospital, Stockholm, Sweden.

出版信息

J Neurol Neurosurg Psychiatry. 1994 Jul;57(7):797-804. doi: 10.1136/jnnp.57.7.797.

Abstract

Electrophysiological data suggest that an abnormal oscillatory pattern of discharge in cortical and thalamic neurons may be the major mechanism underlying primary generalised epilepsy. No neurochemical or anatomical substrate for this theory has hitherto been demonstrated in humans and the pathophysiology of primary generalised epilepsy remains unknown. By means of PET and the benzodiazepine (BZ) ligand [11C]flumazenil it has been previously shown that the BZ receptor density is reduced in the epileptic foci of patients with partial epilepsy. In the present study the method was further developed and used in a comparative analysis of cortical, cerebellar, and subcortical BZ receptor binding in patients with primary generalised tonic and clonic seizures (n = 8), and healthy controls (n = 8). Patients with generalised seizures had an increased BZ receptor density in the cerebellar nuclei (p = 0.006) and decreased density in the thalamus (p = 0.003). No significant changes were seen in the cerebral and cerebellar cortex or in the basal ganglia. The observed alterations suggest that the gamma-amino-butyric acid (GABA)-BZ system may be affected in the cerebello-thalamocortical loop of patients with generalised epilepsy and indicate possible targets for selective pharmacological treatment.

摘要

电生理数据表明,皮质和丘脑神经元放电的异常振荡模式可能是原发性全身性癫痫的主要发病机制。迄今为止,尚未在人类中证实该理论的神经化学或解剖学基础,原发性全身性癫痫的病理生理学仍然未知。通过正电子发射断层扫描(PET)和苯二氮䓬(BZ)配体[11C]氟马西尼,先前已表明部分癫痫患者癫痫病灶中的BZ受体密度降低。在本研究中,该方法得到进一步发展,并用于对原发性全身性强直阵挛发作患者(n = 8)和健康对照者(n = 8)的皮质、小脑和皮质下BZ受体结合进行比较分析。全身性发作患者小脑核中的BZ受体密度增加(p = 0.006),丘脑中的密度降低(p = 0.003)。大脑和小脑皮质以及基底神经节未见明显变化。观察到的改变表明,γ-氨基丁酸(GABA)-BZ系统可能在全身性癫痫患者的小脑-丘脑-皮质环路中受到影响,并提示了选择性药物治疗的可能靶点。

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