中华物理医学与康复杂志
中華物理醫學與康複雜誌
중화물리의학여강복잡지
CHINESE JOURNAL OF PHYSICAL MEDICINE AND REHABILITATION
2014年
4期
250-254
,共5页
左健%贺慧艳%王倩倩%尹娜%谢成娟%王玉
左健%賀慧豔%王倩倩%尹娜%謝成娟%王玉
좌건%하혜염%왕천천%윤나%사성연%왕옥
癫痫%经皮三叉神经电刺激%神经保护%谷氨酸脱羧酶
癲癇%經皮三扠神經電刺激%神經保護%穀氨痠脫羧酶
전간%경피삼차신경전자격%신경보호%곡안산탈최매
Epilepsy%Transcutaneous electrical stimulation%Trigeminal nerve%Neuroprotection%Glutamic acid decarboxylase 65/67
目的 观察经皮三叉神经电刺激对匹罗卡品诱发癫痫持续状态(SE)大鼠海马神经元的保护作用及对大鼠谷氨酸脱羧酶(GAD65/67)表达的影响.方法 通过匹罗卡品建立癫痫点燃模型(即慢性癫痫模型),采用随机数字表法将其分为治疗组及模型组,同时选取正常大鼠纳入空白对照组进行对照.治疗组及模型组大鼠于制模后分别给予三叉神经电刺激或假刺激持续1个月.于电刺激结束并再次诱发SE后6h、24 h、48 h及72 h分别采用TUNNEL和Nissl染色观察各组大鼠SE后海马神经元原位凋亡及脱失情况;于电刺激结束后24 h、72 h、1周、2周及4周时分别采用免疫组化法检测各组大鼠GAD65/67表达情况.结果 SE后24 h、48 h及72 h治疗组海马区TUNNEL阳性细胞、Nissl受损细胞均较模型组显著减少(P<0.05),并以SE后72 h治疗组减少幅度尤为显著(P<0.05).电刺激结束后24 h、72 h、1周、2周及4周时治疗组GAD65/67表达均较模型组明显增强(P<0.05),治疗组GAD65于电刺激结束72h~1周时达到峰值,随后缓慢下降,于电刺激结束4周时接近正常水平.治疗组及模型组大鼠GAD67表达均未见明显峰值,治疗组GAD67表达至电刺激结束4周时仍显著强于模型组水平(P<0.05).结论 经皮三叉神经电刺激治疗对癫痫大鼠海马神经细胞具有保护作用,增强脑内抑制功能可能是其发挥脑保护及抗癫痫作用机制之一.
目的 觀察經皮三扠神經電刺激對匹囉卡品誘髮癲癇持續狀態(SE)大鼠海馬神經元的保護作用及對大鼠穀氨痠脫羧酶(GAD65/67)錶達的影響.方法 通過匹囉卡品建立癲癇點燃模型(即慢性癲癇模型),採用隨機數字錶法將其分為治療組及模型組,同時選取正常大鼠納入空白對照組進行對照.治療組及模型組大鼠于製模後分彆給予三扠神經電刺激或假刺激持續1箇月.于電刺激結束併再次誘髮SE後6h、24 h、48 h及72 h分彆採用TUNNEL和Nissl染色觀察各組大鼠SE後海馬神經元原位凋亡及脫失情況;于電刺激結束後24 h、72 h、1週、2週及4週時分彆採用免疫組化法檢測各組大鼠GAD65/67錶達情況.結果 SE後24 h、48 h及72 h治療組海馬區TUNNEL暘性細胞、Nissl受損細胞均較模型組顯著減少(P<0.05),併以SE後72 h治療組減少幅度尤為顯著(P<0.05).電刺激結束後24 h、72 h、1週、2週及4週時治療組GAD65/67錶達均較模型組明顯增彊(P<0.05),治療組GAD65于電刺激結束72h~1週時達到峰值,隨後緩慢下降,于電刺激結束4週時接近正常水平.治療組及模型組大鼠GAD67錶達均未見明顯峰值,治療組GAD67錶達至電刺激結束4週時仍顯著彊于模型組水平(P<0.05).結論 經皮三扠神經電刺激治療對癲癇大鼠海馬神經細胞具有保護作用,增彊腦內抑製功能可能是其髮揮腦保護及抗癲癇作用機製之一.
목적 관찰경피삼차신경전자격대필라잡품유발전간지속상태(SE)대서해마신경원적보호작용급대대서곡안산탈최매(GAD65/67)표체적영향.방법 통과필라잡품건립전간점연모형(즉만성전간모형),채용수궤수자표법장기분위치료조급모형조,동시선취정상대서납입공백대조조진행대조.치료조급모형조대서우제모후분별급여삼차신경전자격혹가자격지속1개월.우전자격결속병재차유발SE후6h、24 h、48 h급72 h분별채용TUNNEL화Nissl염색관찰각조대서SE후해마신경원원위조망급탈실정황;우전자격결속후24 h、72 h、1주、2주급4주시분별채용면역조화법검측각조대서GAD65/67표체정황.결과 SE후24 h、48 h급72 h치료조해마구TUNNEL양성세포、Nissl수손세포균교모형조현저감소(P<0.05),병이SE후72 h치료조감소폭도우위현저(P<0.05).전자격결속후24 h、72 h、1주、2주급4주시치료조GAD65/67표체균교모형조명현증강(P<0.05),치료조GAD65우전자격결속72h~1주시체도봉치,수후완만하강,우전자격결속4주시접근정상수평.치료조급모형조대서GAD67표체균미견명현봉치,치료조GAD67표체지전자격결속4주시잉현저강우모형조수평(P<0.05).결론 경피삼차신경전자격치료대전간대서해마신경세포구유보호작용,증강뇌내억제공능가능시기발휘뇌보호급항전간작용궤제지일.
Objective To study any protection against hippocampal neuron damage induced by epilepsy (SE) provided by transcutaneous stimulation (TNS) of the trigeminal nerve and to document any effect of such stimulation on the expression of glutamic acid decarboxylase (GAD) 65/67.Methods Pilocarpine injection was used to induce epilepsy in healthy male Sprague-Dawley rats which were then randomly divided into a treatment group and a model group.Rats which had not received the pilocarpine injection served as normal controls.In the treatment group the rats were given electrostimulation for one month after the first spontaneous seizure following the injection of pilocarpine.In the model group they were given sham TNS for one month.After the month of stimula-tion,immunohistochemistry was used to detect the expression of GAD65/67 in the hippocampus.Terminal deoxy-nucleotidyl transferase-mediated dUTP nick end labeling (TUNEL) assays and Nissl staining were applied to deter-mine apoptosis and neuron loss in the hippocampus.Results Significantly less apoptosis was observed in the treatment group than in model group at 24 h,48 h and 72 h post-injection.Compared to the model group,average GAD65/67 expression had increased significantly in the treatment group at 24 h,72 h,1 week,2 weeks and 4 weeks post-stimulation.GAD65 expression reached its peak from 72 h to 1 week post-stimulation,then decreased to the level of the control group by 4 weeks post-stimulation.The expression of GAD67 remained elevated at all the time points employed.Conclusions TNS can significantly protect hippocampal neurons from damage in epilepsy,at least in rats.The underlying anti-epileptic and neuroprotective mechanisms may involve increased inhibitory transmission induced by the stimulation.
