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1����、幼鼠癲癇持續(xù)狀態(tài)成年后腦內(nèi)髓鞘變化的研究劉淑丹1,張桂禎2��,王晗知1�,何揚(yáng)濤1,肖嵐1����,李紅麗1(400038重慶�����,第三軍醫(yī)大學(xué)基礎(chǔ)醫(yī)學(xué)部組織學(xué)與胚胎學(xué)教研室1�����,610083成都,成都軍區(qū)總醫(yī)院信息科2)[摘要]目的探討致癲癇持續(xù)狀態(tài)幼鼠(statusepilepticus����,SE)成年后發(fā)展為自發(fā)反復(fù)性癲癇發(fā)作(spontaneousrecurrentepilepticseizure,SRS)的大鼠腦內(nèi)髓鞘的變化�。方法采用氯化鋰-匹羅卡品腹腔注射誘P20-P28體重(70±5)g雄性SD幼鼠SE模型,應(yīng)用多道生理信號(hào)采集處理系統(tǒng)檢測大鼠腦電圖(electroencephalogra
2�����、m��,EEG)異?����;顒?dòng)波����,采用Nissl染色方法觀察腦內(nèi)神經(jīng)元的變化,證實(shí)SRS模型大鼠誘導(dǎo)成功�;應(yīng)用盧卡斯快藍(lán)(luxolfastblue,LFB)染色及髓鞘堿性蛋白(myelinbasicprotein��,MBP)免疫組織化學(xué)染色等技術(shù)觀察腦內(nèi)髓鞘的變化。結(jié)果SRS模型組腦電圖與正常對照組相比�,可見頻發(fā)尖波、棘-慢���、尖-慢綜合波��;Nissl染色顯示神經(jīng)元數(shù)目在海馬CA1(242.1±33.6)����、CA3(354.8±26.8)和齒狀回門區(qū)(61.8±8.3)減少(P<0.01)��,部分細(xì)胞變性和壞死���。LFB染色可見SRS模型組在胼胝體(callosumcorpus�����,cc�����;0.162±0
3、.017)����、扣帶回(cingulatedgyrus�����,cg�����;0.139±0.013)與海馬白質(zhì)(0.080±0.007)區(qū)域內(nèi)的著色范圍明顯縮小���,著色淺淡,與正常對照組相比有顯著差異(P<0.01)����;MBP免疫陽性沉淀在cc(0.183±0.013)、cg(0.192±0.016)���、第一軀體感覺皮質(zhì)區(qū)(S1BF�;0.076±0.012)和第一聽皮質(zhì)區(qū)(Au1��;0.085±0.014)內(nèi)的平均光密度值(OD)顯著低于正常對照組(P<0.01)���。結(jié)論致癇幼鼠成年后伴有慢性癲癇發(fā)作可造成中樞神經(jīng)系統(tǒng)髓鞘脫失�。[關(guān)鍵詞]氯化鋰-匹羅卡品;慢性癲癇���;腦電圖���;脫髓鞘;髓鞘堿性蛋白[中圖法分類號(hào)]
4��、[文獻(xiàn)標(biāo)志碼]AStudyonChangesofmyelinofratsinducedstatusepilepticusinjuvenilestageLIUShu-dan,ZHANGGuizhen,WANGHan-zhi,HEYang-tao,XIAOLan,LIHong-li(1DepartmentofHistologyandEmbryology,ThirdMilitaryMedicalUniversity,Chongqing400038,2DepartmentofInformatics,GeneralHospitalofChengduMilitaryCommand,Chengd
5����、u,SichuanProvince,610083)[Abstract]ObjectiveToinvestigatethechangeofmyelininthebrainofthematureratswithspontaneousrecurrentepilepticseizure(SRS)afterinducedstatusepilepticus(SE)inimmature.MethodsThemodelofP21-P28wight(70±5)gmalejuvenilSEratswasinducedbylithium–pilocarpineadministration.Electro
6、encephalogram(EEG)wasusedtomonitortheabnormalwaveofepilepsy���;Nisslstainingwasusedtoobservethealterationofneuroninhippocampus.ThenLuxolFastblue(LFB)stainingandtheexpressionsofmyelinbasicprotein(MBP)werestudiedbyhistopathologicalandimmunohistochemistrymethods.ResultsTheEEGandNisslstainingconfirme
7����、dtheratswereinducedsuccessfullytoSRSmodel��;thepositiveLFBstainingofthemodelgroupturnedtolighterandsmallerespeciallyinthecallosumcorpus(cc)�����,cingulatedgyrus(cg)andwhitematterofhippocampus(P<0.01).Theaverageopticaldensity(OD)ofMBPpositivear
