丘脑前核电刺激可抑制戊四氮点燃大鼠,并伴随腺苷激酶表达降低。
Deep brain stimulation of the anterior thalamus attenuates PTZ kindling with concomitant reduction of adenosine kinase expression in rats.
机构信息
Department of Physiology, Universidade Federal de Sao Paulo, Sao Paulo, Brazil.
Department of Neurosurgery, Jersey Shore University Medical Center, Hackensack Meridian Health Network, Neptune, NJ, USA.
出版信息
Brain Stimul. 2022 Jul-Aug;15(4):892-901. doi: 10.1016/j.brs.2022.05.020. Epub 2022 Jun 8.
BACKGROUND
Deep brain stimulation (DBS) of the anterior nucleus of the thalamus (ANT) is an emerging therapy to provide seizure control in patients with refractory epilepsy, although its therapeutic mechanisms remain elusive.
OBJECTIVE
We tested the hypothesis that ANT-DBS might interfere with the kindling process using three experimental groups: PTZ, DBS-ON and DBS-OFF.
METHODS
79 male rats were used in two experiments and exposed to chemical kindling with pentylenetetrazole (PTZ, 30 mg/kg i.p.), delivered three times a week for a total of 18 kindling days (KD). These animals were divided into two sets of three groups: PTZ (n = 26), DBS-ON (n = 28) and DBS-OFF (n = 25). ANT-DBS (130 Hz, 90 μs, and 200 μA) was paired with PTZ injections, while DBS-OFF group, although implanted remained unstimulated. After KD 18, the first set of PTZ-treated animals and an additional group of 11 naïve rats were euthanized for brain extraction to study adenosine kinase (ADK) expression. To observe possible long-lasting effects of ANT stimulation, the second set of animals underwent a 1-week treatment and stimulation-free period after KD 18 before a final PTZ challenge.
RESULTS
ANT-DBS markedly attenuated kindling progression in the DBS-ON group, which developed seizure scores of 2.4 on KD 13, whereas equivalent seizure scores were reached in the DBS-OFF and PTZ groups as early as KD5 and KD6, respectively. The incidence of animals with generalized seizures following 3 consecutive PTZ injections was 94%, 74% and 21% in PTZ, DBS-OFF and DBS-ON groups, respectively. Seizure scores triggered by a PTZ challenge one week after cessation of stimulation revealed lasting suppression of seizure scores in the DBS-ON group (2.7 ± 0.2) compared to scores of 4.5 ± 0.1 for the PTZ group and 4.3 ± 0.1 for the DBS-OFF group (P = 0.0001). While ANT-DBS protected hippocampal cells, the expression of ADK was decreased in the DBS-ON group compared to both PTZ (P < 0.01) and naïve animals (P < 0.01).
CONCLUSIONS
Our study demonstrates that ANT-DBS interferes with the kindling process and reduced seizure activity was maintained after a stimulation free period of one week. Our findings suggest that ANT-DBS might have additional therapeutic benefits to attenuate seizure progression in epilepsy.
背景
丘脑前核深部脑刺激(DBS)是一种新兴的治疗方法,可提供对难治性癫痫患者的癫痫控制,尽管其治疗机制仍不清楚。
目的
我们测试了这样一种假设,即 ANT-DBS 可能通过三个实验组(PTZ、DBS-ON 和 DBS-OFF)来干扰点燃过程。
方法
79 只雄性大鼠用于两项实验,并接受戊四氮(PTZ,30mg/kg ip)的化学点燃,每周三次,共进行 18 次点燃日(KD)。这些动物被分为两组三个亚组:PTZ(n=26)、DBS-ON(n=28)和 DBS-OFF(n=25)。ANT-DBS(130Hz、90μs 和 200μA)与 PTZ 注射配对,而 DBS-OFF 组虽然植入但未受刺激。KD18 后,第一组 PTZ 处理的动物和另外 11 只未处理的大鼠被安乐死,以提取大脑,研究腺苷激酶(ADK)的表达。为了观察 ANT 刺激的可能长期影响,第二组动物在 KD18 后进行了为期一周的治疗和刺激无治疗期,然后进行了最后的 PTZ 挑战。
结果
ANT-DBS 显著抑制了 DBS-ON 组的点燃进展,DBS-ON 组在 KD13 时的发作评分达到 2.4,而 DBS-OFF 组和 PTZ 组分别在 KD5 和 KD6 时达到相同的发作评分。在 3 次连续 PTZ 注射后,动物出现全面性发作的发生率分别为 94%、74%和 21%,分别为 PTZ、DBS-OFF 和 DBS-ON 组。在刺激停止一周后,PTZ 引发的发作评分显示,DBS-ON 组的发作评分持续抑制(2.7±0.2),而 PTZ 组和 DBS-OFF 组的发作评分分别为 4.5±0.1 和 4.3±0.1(P=0.0001)。虽然 ANT-DBS 保护海马细胞,但与 PTZ(P<0.01)和未处理的动物(P<0.01)相比,DBS-ON 组的 ADK 表达减少。
结论
我们的研究表明,ANT-DBS 干扰了点燃过程,并且在刺激停止一周后的无刺激期内,减少的发作活动仍然持续。我们的发现表明,ANT-DBS 可能具有额外的治疗益处,以减轻癫痫的发作进展。
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