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《TrkB信号通路调控的研究.pdf》由会员上传分享,免费在线阅读,更多相关内容在行业资料-天天文库。
1、TianjinMedJ,May2014,Vol42No5TrkB同亚型对癫痫海马神经元BDNF/TrkB信号通路调控的研究吴秋静常伟潘立平宋毅军赵文【摘要】目的探讨癫痫海马神经元中酪氨酸激酶受体B(TrkB)不同亚型对脑源性神经营养因子(BDNF)/TrkB信号通路的调控机制。方法取原代培养7d后的海马神经元,分为钙调蛋白抑制剂(ALLN)组和翻译抑制剂(An—isomycin)两大组。ALLN组又分为正常组、正常+BNDF组、癫痫组、癫痫+BDNF组、正常+ALLN组、癫痫+ALLN组和癫痫+ALLN+BDNF~;Anisomvcin组又分为正常组、正常+BDNF组、癫痫组
2、、癫痫+BDNF组、正常+Anisomycin组、癫痫+Anisomvcin组和癫痫+Anisomycin+BDNF组。免疫荧光鉴定海马神经元,无镁液处理制备癫痫模型,电生理鉴定细胞痫样放电,免疫印迹技术检测各组TrkB和磷酸化TrkB(p—TrkB)蛋白的表达变化。结果(1)ALLN组:正常+BDNF组p—TrkB/TrkB灰度值高于正常组;癫痫+BDNF组高于癫痫组,低于正常+BDNF组;癫痫+ALLN+BDNF组低于癫痫+BDNF组,与癫痫+ALLN组差异无统计学意义。(2)Anisomycin组:正常+BDNF组p-TrkB/TrkB灰度值高于正常组;癫痫+BDNF组
3、高于癫痫组,低于正常+BDNF组;癫痫+Anisomycin+BDNF组高于癫痫+BDNF组和癫痫+Anisomy—cin组。结论通过Anisomycin降低TrkB.T表达可改善癫痫状态下BDNF/TrkB受抑制的状态,通过ALLN升高TrkB.FL表达无法改善其抑制状态。【关键词】癫痫,颞叶;受体,TrkB;脑源性神经营养因子;茴香霉素;海马;神经元;钙调蛋白抑制剂【中图分类号】R742.1【文献标识码】A【DOI】10.3969/jAssn.0253—9896.2014.05.002AnExperimentalStudyoftheRegulationofBDNF/Trk
4、BSignalPathwaybyDifferentIsoformsofTrkBjnEpilepticHippocampalNeuronswuQiujing,CHANGWei,PANLiping,SONGYijun,ZHAOWenDepartmentofNeurology,theGeneralHospitalofTianjinMedicalUniversity,Tianjin300052,China【Abstract】0bjectiveToinvestigatethemechanismofbrainderivedneurotrophicfactor(BDNF)regulated
5、bydiffer—entisoformsoftyrosinekinasereceptorB(TrkB)inepileptichippocampalneurons.MethodsPrimaryhippocampalneu·ronswereculturedinvitrofor7days,anddividedintotwogroups,ALLN(calcineurininhibitor)groupandAnisomycin(trans—lationinhibitor)group.ALLNgroupincludedcontrolgroup,control+BDNFgroup,epil
6、epsygroup,epilepsy+BDNFgroup,control+ALLNgroup,epilepsy+ALLNgroupandepilepsy+ALLN+BDNFgroup.Anisomycingroupwassub—dividedintocon—trolgroup,control+BDNFgroup,epilepsygroup,epilepsy+BDNFgroup,contml+Anisomycingroup,epilepsy+Anisomycingroupandepilepsy+Anisomycin+BDNFgroup.Theimmunofluorescentt
7、echniquewasusedtoidentificatethehippocampalneurons.Epileptiformdischargesweredetectedbyelectrophysiol0gica1techniques.Westernblotassaywasusedtodeter—minetheproteinexpressionofTrkBandphosphorylatedTrkB(p—TrkB)inallcellgroups.Results(1)InALLNgroup,thegrayv
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