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托吡酯对早期发育期间反复和长时间癫痫发作的影响。

Effect of topiramate following recurrent and prolonged seizures during early development.

作者信息

Cha Byung Ho, Silveira Diosely C, Liu Xianzeng, Hu Yingchun, Holmes Gregory L

机构信息

Clinical Neurophysiology Laboratory, Department of Neurology, Center for Research in Pediatric Epilepsy, Harvard Medical School, Children's Hospital Boston, Hunnewell 2, 300 Longwood Avenue, Boston, MA 02115, USA.

出版信息

Epilepsy Res. 2002 Oct;51(3):217-32. doi: 10.1016/s0920-1211(02)00157-2.

Abstract

Topiramate, an antiepileptic drug with a number of mechanisms of action including inhibition of glutamate activity at the AMPA and KA receptors, was assessed as a neuroprotective agent following seizures. We administered topiramate, 80 mg/kg, or saline for 4 weeks following a series of 25 neonatal seizures or status epilepticus (SE) induced by lithium-pilocarpine in postnatal day 20 rats. Age-matched control rats without a history of seizures were administered topiramate or saline. Following completion of the topiramate injections, animals were tested in the water maze for spatial learning and the brains examined for cell loss and sprouting of mossy fibers. While there was a trend for improved visual-spatial performance in the water maze following topiramate therapy in rats with neonatal seizures, no differences were found in the histological examination of the hippocampus. Neonatal rats exposed to 4 weeks of topiramate did not differ from non-treated controls in water maze performance or histological examination. In weanling rats subjected to SE, topiramate provided a moderate degree of neuroprotection, with topiramate-treated rats performing better in the water maze than rats receiving saline. However, no differences in cell loss or mossy fiber sprouting were found in the histological examination of the brains. These findings demonstrate that chronic treatment with topiramate following SE improves cognitive function. In addition, long-term administration of high-dose topiramate in the normal developing rat brain does not appear to impair cognitive performance.

摘要

托吡酯是一种具有多种作用机制的抗癫痫药物,包括抑制AMPA和KA受体处的谷氨酸活性,在癫痫发作后被评估为一种神经保护剂。我们在出生后第20天的大鼠中,通过锂-匹鲁卡品诱导一系列25次新生儿癫痫发作或癫痫持续状态(SE)后,给予托吡酯80mg/kg或生理盐水,持续4周。对无癫痫发作史的年龄匹配对照大鼠给予托吡酯或生理盐水。在完成托吡酯注射后,对动物进行水迷宫空间学习测试,并检查大脑中的细胞丢失和苔藓纤维发芽情况。虽然新生儿癫痫大鼠接受托吡酯治疗后在水迷宫中的视觉空间表现有改善趋势,但在海马组织学检查中未发现差异。暴露于4周托吡酯的新生大鼠在水迷宫表现或组织学检查方面与未治疗的对照大鼠没有差异。在经历SE的断奶大鼠中,托吡酯提供了中度的神经保护作用,接受托吡酯治疗的大鼠在水迷宫中的表现优于接受生理盐水的大鼠。然而,在大脑组织学检查中未发现细胞丢失或苔藓纤维发芽的差异。这些发现表明,SE后长期使用托吡酯治疗可改善认知功能。此外,在正常发育的大鼠脑中长期给予高剂量托吡酯似乎不会损害认知表现。

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