Acute induction of epileptiform discharges by pilocarpine in the in vitro isolated guinea-pig brain requires enhancement of blood-brain barrier permeability.

Uva L; Librizzi L; Marchi N; Noe F; Bongiovanni R; Vezzani A; Janigro D; de-Curtis M

首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Acute induction of epileptiform discharges by pilocarpine in the in vitro isolated guinea-pig brain requires enhancement of blood-brain barrier permeability.

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Acute induction of epileptiform discharges by pilocarpine in the in vitro isolated guinea-pig brain requires enhancement of blood-brain barrier permeability.

机译：毛果芸香碱在体外分离的豚鼠脑中急性诱发癫痫样放电需要增强血脑屏障通透性。

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Systemic application of the muscarinic agonist, pilocarpine, is commonly utilized to induce an acute status epilepticus that evolves into a chronic epileptic condition characterized by spontaneous seizures. Recent findings suggest that the status epilepticus induced by pilocarpine may be triggered by changes in the blood-brain barrier (BBB) permeability. We tested the role of the BBB in an acute pilocarpine model by using the in vitro model brain preparation and compared our finding with in vivo data. Arterial perfusion of the in vitro isolated guinea-pig brain with <1 mM pilocarpine did not cause epileptiform activity, but rather reduced synaptic transmission and induced steady fast (20-25 Hz) oscillatory activity in limbic cortices. These effects were reversibly blocked by co-perfusion of the muscarinic antagonist atropine sulfate (5 microM). Brain pilocarpine measurements in vivo and in vitro suggested modest BBB penetration. Pilocarpine induced epileptiform discharges only when perfused with compounds that enhance BBB permeability, such as bradykinin (n=2) or histamine (n=10). This pro-epileptic effect was abolished when the BBB-impermeable muscarinic antagonist atropine methyl bromide (5 microM) was co-perfused with histamine and pilocarpine. In the absence of BBB permeability enhancing drugs, pilocarpine induced epileptiform activity only after arterial perfusion at concentrations >10 mM. Ictal discharges correlated with a high intracerebral pilocarpine concentration measured by high pressure liquid chromatography. We propose that acute epileptiform discharges induced by pilocarpine treatment in the in vitro isolated brain preparation are mediated by a dose-dependent, atropine-sensitive muscarinic effect promoted by an increase in BBB permeability. Pilocarpine accumulation secondary to BBB permeability changes may contribute to in vivo ictogenesis in the pilocarpine epilepsy model.

机译：毒蕈碱激动剂毛果芸香碱的系统性应用通常被用来诱导急性状态的癫痫病，其发展为以自发性癫痫为特征的慢性癫痫病。最近的发现表明，毛果芸香碱引起的癫痫持续状态可能是由血脑屏障（BBB）通透性的改变引起的。我们使用体外模型脑准备测试了BBB在急性毛果芸香碱模型中的作用，并将我们的发现与体内数据进行了比较。小于1 mM毛果芸香碱体外离体的豚鼠脑的动脉灌注未引起癫痫样活动，但减少了突触传递并在边缘皮质中诱导了稳定的快速（20-25 Hz）振荡活动。毒蕈碱性拮抗剂硫酸阿托品（5 microM）的共同灌注可逆地阻断了这些作用。体内和体外脑毛细芸苔素的测量表明适度的血脑屏障渗透。毛果芸香碱诱导的癫痫样放电仅在灌注增强BBB通透性的化合物（如缓激肽（n = 2）或组胺（n = 10））时释放。当将BBB不可渗透的毒蕈碱拮抗剂阿托品甲基溴（5 microM）与组胺和毛果芸香素共同灌注时，这种抗癫痫的作用就消失了。在缺乏BBB通透性增强药物的情况下，毛果芸香碱仅在浓度> 10 mM的动脉灌注后才诱导癫痫样活动。局部放电与高压液相色谱法测得的脑内毛果芸香碱浓度高有关。我们建议通过毛果芸香碱治疗在体外分离的脑准备中诱导的急性癫痫样放电是由BBB通透性增加促进的剂量依赖性阿托品敏感毒蕈碱作用介导的。 BBB通透性变化继发的毛果芸香碱积累可能在毛果芸香碱癫痫模型中促成体内信息生成。

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来源
《Neuroscience: An International Journal under the Editorial Direction of IBRO》 |2008年第1期|共10页
作者
Uva L; Librizzi L; Marchi N; Noe F; Bongiovanni R; Vezzani A; Janigro D; de-Curtis M;
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正文语种 eng
中图分类人体生理学;
关键词
Pilocarpine; Blood-Brain Barrier; In Vitro; Acute; 毛果芸香碱; 血脑屏障;

机译：Pilocarpine;Blood-Brain Barrier;In Vitro;Acute;毛果芸香碱;血脑屏障;

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机译：毛果芸香碱在体外分离的豚鼠脑中急性诱发癫痫样放电需要增强血脑屏障通透性。
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Acute induction of epileptiform discharges by pilocarpine in the in vitro isolated guinea-pig brain requires enhancement of blood-brain barrier permeability.

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