首页> 外文期刊>Epilepsy research >Quantitative evaluation of central-type benzodiazepine receptors with ((125)I) Iomazenil in experimental epileptogenesis I. The rat kainate model of temporal lobe epilepsy.
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Quantitative evaluation of central-type benzodiazepine receptors with ((125)I) Iomazenil in experimental epileptogenesis I. The rat kainate model of temporal lobe epilepsy.

机译:定量评价实验性癫痫发生中具有((125)I)咪唑的中心型苯并二氮杂receptor受体I.大鼠颞叶癫痫的海藻酸盐模型。

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This study aimed at quantitatively evaluating hippocampal central-type benzodiazepine receptors (BZRs) in the kainate model of temporal lobe epilepsy (TLE) by in vitro autoradiography (ARG) using [(125)I] Iomazenil (IMZ) specific ligand for central-type BZRs. Kainate (1microg/0.5microl) was injected into the left amygdala to induce limbic status epilepticus. One, three, or six months after injection, in vitro ARG with [(125)I] IMZ and cell counts were performed in the hippocampal CA1-4 regions and dentate gyrus ipsilateral to the kainate injection site, and were compared with the vehicle-injected control group. In all kainate-treated rats, clear pyramidal neuron loss was observed in left hippocampal areas CA1-4. Compared with the control group, progressive reduction of [(125)I] IMZ binding was also observed. This resulted in a marked binding decrease paralleling pyramidal neuron loss in hippocampal areas CA1 (down to 83% of control), CA2 (76%), CA3 (75%), and CA4 (90%) at 6 months after kainate administration. Conversely, [(125)I] IMZ binding significantly increased in the dentate gyrus (up to 106% of control) at 1 month, but returned to nearly normal at 3-6 months. These results suggest that central-type BZR neuroimaging is useful in detecting hippocampal sclerosis in the mesial TLE, though central BZR alterations differ depending on hippocampal subfields and post-seizure time-courses.
机译:这项研究旨在通过体外放射自显影(ARG)使用[(125)I]咪唑醇(IMZ)特异性中枢型配体对体外颞叶癫痫(TLE)海地模型中的海马中枢型苯二氮卓受体(BZRs)进行定量评估BZR。向左杏仁核注射海因酸盐(1microg / 0.5microl)以诱发边缘性癫痫发作。注射后1,3或6个月,在海马CA1-4区和海藻酸盐注射部位的齿状回同侧进行[[125] I] IMZ和细胞计数的体外ARG,并与溶媒比较-注射对照组。在所有用海藻酸盐治疗的大鼠中,在左海马区CA1-4中观察到明显的锥体神经元丢失。与对照组相比,还观察到[(125)I] IMZ结合的进行性降低。这导致在海藻酸盐给药后6个月,海马区CA1(下降至对照组的83%),CA2(76%),CA3(75%)和CA4(90%)的锥体细胞神经元损失明显减少。相反,[(125)I] IMZ结合在1个月时在齿状回中显着增加(高达对照的106%),但在3-6个月时恢复到接近正常。这些结果表明,中央型BZR神经影像学可用于检测中TLE的海马硬化,尽管中央型BZR改变取决于海马亚域和发作后的时程。

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