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双侧和单侧将产生 GABA 的细胞移植到丘脑底核对急性癫痫模型的抗惊厥作用。

Anticonvulsant effects by bilateral and unilateral transplantation of GABA-producing cells into the subthalamic nucleus in an acute seizure model.

机构信息

Department of Pharmacology, Toxicology, and Pharmacy, University of Veterinary Medicine, Hannover, Germany.

出版信息

Cell Transplant. 2014 Jan;23(1):111-32. doi: 10.3727/096368912X658944. Epub 2012 Nov 27.

Abstract

Neural transplantation of GABA-producing cells into key structures within seizure-suppressing circuits holds promise for medication-resistant epilepsy patients not eligible for resection of the epileptic focus. The substantia nigra pars reticulata (SNr), a basal ganglia output structure, is well known to modulate different seizure types. A recent microinjection study by our group indicated that the subthalamic nucleus (STN), which critically regulates nigral activity, might be a more promising target for focal therapy in epilepsies than the SNr. As a proof of principle, we therefore assessed the anticonvulsant efficacy of bilateral and unilateral allografting of GABA-producing cell lines into the STN using the timed intravenous pentylenetetrazole seizure threshold test, which allows repeated seizure threshold determinations in individual rats. We observed (a) that grafted cells survived up to the end of the experiments, (b) that anticonvulsant effects can be induced by bilateral transplantation into the STN using immortalized GABAergic cells derived from the rat embryonic striatum and cells additionally transfected to obtain higher GABA synthesis than the parent cell line, and (c) that anticonvulsant effects were observed even after unilateral transplantation into the STN. Neither grafting of control cells nor transplantation outside the STN induced anticonvulsant effects, emphasizing the site and cell specificity of the observed anticonvulsant effects. To our knowledge, the present study is the first showing anticonvulsant effects by grafting of GABA-producing cells into the STN. The STN can be considered a highly promising target region for modulation of seizure circuits and, moreover, has the advantage of being clinically established for functional neurosurgery.

摘要

将产生 GABA 的细胞神经移植到抑制癫痫发作的关键结构中,为不符合切除癫痫病灶标准的耐药性癫痫患者带来了希望。黑质网状部(SNr)是基底神经节的输出结构,众所周知,它可以调节不同类型的癫痫发作。我们小组最近的一项微注射研究表明,丘脑底核(STN)作为黑质活动的关键调节部位,可能比 SNr 更适合作为癫痫灶局部治疗的靶点。作为一个原理验证,我们因此使用戊四氮静脉注射癫痫发作阈测试评估了将产生 GABA 的细胞系移植到 STN 双侧和单侧的抗惊厥效果,该测试允许在个体大鼠中重复测定癫痫发作阈。我们观察到:(a)移植的细胞存活到实验结束;(b)使用源自大鼠胚胎纹状体的永生化 GABA 能细胞和另外转染以获得比亲本细胞系更高 GABA 合成的细胞进行双侧 STN 移植可以诱导抗惊厥作用;(c)即使在 STN 单侧移植后也观察到抗惊厥作用。移植对照细胞或移植到 STN 以外均不会引起抗惊厥作用,强调了观察到的抗惊厥作用的部位和细胞特异性。据我们所知,本研究首次证明了将产生 GABA 的细胞移植到 STN 可产生抗惊厥作用。STN 可被视为调节癫痫发作回路的极具前途的靶点,而且,它具有已被临床确立用于功能性神经外科手术的优势。

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