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腹侧苍白球深部脑刺激可减轻两种大鼠模型中的急性部分性、全身性和强直阵挛性癫痫发作。

Ventral pallidum deep brain stimulation attenuates acute partial, generalized and tonic-clonic seizures in two rat models.

作者信息

Mahoney Emily C, Zeng Andrew, Yu Wilson, Rowe Mackenzie, Sahai Siddhartha, Feustel Paul J, Ramirez-Zamora Adolfo, Pilitsis Julie G, Shin Damian S

机构信息

Department of Neuroscience & Experimental Therapeutics, Albany Medical College, Albany NY, United States.

Department of Neuroscience, University of Minnesota, Minneapolis MN, United States.

出版信息

Epilepsy Res. 2018 May;142:36-44. doi: 10.1016/j.eplepsyres.2018.03.010. Epub 2018 Mar 9.

Abstract

Approximately 30% of individuals with epilepsy are refractory to antiepileptic drugs and currently approved neuromodulatory approaches fall short of providing seizure freedom for many individuals with limited utility for generalized seizures. Here, we expand on previous findings and investigate whether ventral pallidum deep brain stimulation (VP-DBS) can be efficacious for various acute seizure phenotypes. For rats administered pilocarpine, we found that VP-DBS (50 Hz) decreased generalized stage 4/5 seizure median frequency from 9 to 6 and total duration from 1667 to 264 s even after generalized seizures emerged. The transition to brainstem seizures was prevented in almost all animals. VP-DBS immediately after rats exhibited their first partial forebrain stage 3 seizure did not affect the frequency of partial seizures but reduced median partial seizure duration from 271 to 54 s. Stimulation after partial seizures also reduced the occurrence and duration of secondarily generalized stage 4/5 seizures. VP-DBS prior to pilocarpine administration prevented the appearance of partial seizures in almost all animals. Lastly, VP-DBS delayed the onset of generalized tonic-clonic seizures (GTCSs) from 111 to 823 s in rats administered another chemoconvulsant, pentylenetetrazol (PTZ, 90 mg/kg). In this particular rat seizure model, stimulating electrodes placed more laterally in both VP hemispheres and more posterior in the left VP hemisphere provided greatest efficacy for GTCSs. In conclusion, our findings posit that VP-DBS can serve as an effective novel neuromodulatory approach for a variety of acute seizure phenotypes.

摘要

大约30%的癫痫患者对抗癫痫药物难治,目前获批的神经调节方法未能使许多患者实现无癫痫发作,对全身性癫痫发作的效用有限。在此,我们扩展先前的研究结果,调查腹侧苍白球深部脑刺激(VP-DBS)对各种急性癫痫发作表型是否有效。对于给予毛果芸香碱的大鼠,我们发现即使在全身性癫痫发作出现后,VP-DBS(50Hz)也能将全身性4/5期癫痫发作的中位频率从9次降至6次,总时长从1667秒降至264秒。几乎所有动物都能防止向脑干癫痫发作的转变。在大鼠首次出现部分性前脑3期癫痫发作后立即进行VP-DBS,并不影响部分性癫痫发作的频率,但可将部分性癫痫发作的中位时长从271秒降至54秒。部分性癫痫发作后进行刺激也可减少继发性全身性4/5期癫痫发作的发生和时长。在给予毛果芸香碱之前进行VP-DBS可防止几乎所有动物出现部分性癫痫发作。最后,在给予另一种化学惊厥剂戊四氮(PTZ,90mg/kg)的大鼠中,VP-DBS将全身性强直阵挛性癫痫发作(GTCSs)的发作起始时间从111秒延迟至823秒。在这个特定的大鼠癫痫模型中,将刺激电极放置在双侧VP半球更外侧以及左侧VP半球更靠后的位置,对GTCSs的疗效最佳。总之,我们的研究结果表明,VP-DBS可作为一种针对各种急性癫痫发作表型的有效的新型神经调节方法。

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