简介:目的:观察电针天柱穴对大鼠颈椎间盘退变组织bcl-2、bcl—XL表达的影响。方法:将40只SD雄性大鼠,随机分为4组,即假手术组、电针组、西药组和模型组,每组10只。除假手术组外,其余3组造成动静力失衡性颈椎间盘退变模型。电针组给予电针天柱穴、大杼穴治疗;西药组用芬必得治疗;模型组造模后不作任何处理。治疗30d后,运用免疫组化法观察各组大鼠椎间盘组织bcl-2、bcl—xL的表达。结果:bcl-2在电针组、假手术组和西药组中表达明显高于模型组(P〈0.01),电针组、假手术组和西药组之间的表达无显著性差异。bcl-XL在电针组的表达低于假手术组(P〈0.01),高于西药组、模型组(P〈0.01)。结论:电针可以提高大鼠退变椎间盘组织bcl-2、bcl—XL的表达,是其延缓椎间盘组织凋亡,发挥治疗作用的可能途径之一。
简介:Objective:ToinvestigatetheexpressionofE2FandBcl-2andtheclinicopathologicalsignificanceinhepatocellularcarcinoma.Methods:TheexpressionsofE2F-3andBcl-2in74patientswithhepaticcarcinoma,paracarcinomaand15patientswithlivercirrhosisweredetectedbyS-Pimmunohistochemicalstaining.Results:TheexpressionofE2Finhepaticcarcinomawassignificantlyhigherthanthatinparacarcinomaorlivercirrhosis(P<0.005),theexpressionofBcl-2inhepaticcarcinomawassignificantlyhigherthanthatinparacarcinoma(P<0.005),inwhichBcl-2expressionwaslowerthaninlivercirrhosis(P<0.05).TheexpressionofE2F-3wasrelatedwithhistologicalgrade,tumorsize,andtheexpressionofBcl-2wasrelatedwithhistologicalgrade,tumorsizeandtumornumber.TherewascorrelationbetweentheexpressionofE2F-3andBcl-2inhepaticcarcinoma.Conclusion:E2F-3andBcl-2expressionmayplayanimportantroleindevelopment,progressionandcellapoptosisoftumor.
简介:Toinvestigatetheexpressionofapoptosis-relatedprotein(Fas,FasL,andBcl-2)inthepathogenesisofautoimmunethyroiddisorders(ATDs),immunohistochemicalstainingwasperformedon20Hashimoto'sthyroiditis(HT),20Graves'disease(GD),and20thyroidfollicularadenoma(TFA,ascontrol).AllthecasesexpressedFas,mainlyonthecellsurfaceandcytoplasm.FasLwasfoundin17casesoftheTFA.Bcl-2wasdetectedin15casesofHT,19ofGDand17ofTFA.InTFA,amoderateFasexpressionandaminimalornoFasLexpressionwasdetectedonfollicularcells.InHT,thefolliclesadjacenttoinfiltratinglymphocytesshowedincreasedlevelsofFasandFasLexpression.AweakerstainingofFasandFasLwasexhibitedoninfiltratinglymphocytesthanonthyrocytes.InacomparisonofGDwithHT,thyrocytesandlymphocytesshowedsimilarFasstaining,butforFasLthestainingwasratherweakerinHT.TheexpressionofBcl-2wasnearlyidenticalinGDandTFA,butmuchweakeronthefollicularcellsinvicinityoflymphocytesandonthelymphocyteslocatedingerminalcentersofHTtissues.TheexpressionofFas,FasL,Bcl-2inHashimoto'sthyroiditisandGraves'diseasewerealmostsame.FasLstrongexpressionandBcl-2weakexpressiononthefolliclesinHTmayinduceapoptosis.TheseresultsprovidedevidenceforexpressionofFas,FasLandBcl-2inthepathogenesisofautoimmunethyroiddisease.ThelymphocytesseemnottobedirectlyengagedintheprocessviatheirownFasL,buttheymayprovidesomecytokinesthat,inturn,upregulateFasand/orFasLexpressiontoinduceapoptosis.
简介:BCL-2 蛋白家族与细胞凋亡.细胞生物学杂志 2001,Caspase家族与细胞凋亡调控,Caspase家族与细胞凋亡
简介:客观:为了学习表达式和apoptosis的临床的价值,在乳癌控制基因bcl-2和bax。方法:在在1996在我们的医院里从操作获得的41乳癌的蛋白质bax和bcl-2与正常的胸纸巾用ABCimmunohistochemical污点试金并且与10个盒子相比被检测。结果:在正常的胸组织的bax的积极的率是90%并且在乳癌是59%,与他们之间的重要统计差别(P<0.05),但是在bcl-2没有统计差别蛋白质表示。在41乳癌之中,有淋巴节点转移(21个盒子)的组有显然低的bax表示(43%)和高bcl-2表示(76%),给没有淋巴节点转移的组显示出重要差别(P<0.05)。结论:bcl-2的antiapoptosis功能是比在乳癌的bax强壮的。蛋白质bax和bcl-2试金可能在理解乳癌的生物行为是有用的。
简介:biflavonoidisochamaejasmin主要在StellerachamaejasmeL的根被散布。(Thymelaeaceae)那在繁体中文药(TCM)被使用治疗肿瘤,肺结核,和干癣。此处,isochamaejasmin被发现对Bcl-2家庭蛋白质显示出类似的bioactivity到参考Bcl-2ligand(−)通过3D类似搜索的-gossypol。它有选择地跳了到Bclx有K和Mcl-1>是的i价值1.93±0.13mol·L−1和9.98±0.21mol·L−1,分别地。另外,isochamaejasmin显示出细微生长对有是的IC50价值的HL-60的禁止的活动50.40±1.21mol·L−1和中等生长对有IC50价值的K562细胞的禁止的活动是24.51±1.62mol·L−1。而且,isochamaejasmin由增加在Bcl-2-inducedapoptosis小径包含了的caspase-9,caspase-3,和PARP的劈开的蛋白质的细胞内部的表示层次导致了K562房间的apoptosis。这些结果显示isochamaejasmin由禁止Bcl-2家庭蛋白质的活动在白血病房间导致apoptosis,提供为进一步学习S的内在的反癌症机制的证据。chamaejasmeL。
简介:Objective:TheexpressionofB-celllymphoma2(Bcl-2)seemstobeinfluencedbytheendocrineenvironment.NumerousreportsdemonstratethediverseexpressionofBcl-2familymembersundersexsteroidregulation.Withtheexceptionofestrogen-relatedtumors,androgen-relatedtumorshaveshowntheircharacteristicsinBcl-2expression.Inthisstudy,thestatusofBcl-2expressioninmalehepatocellularcarcinoma(HCC)patientswasexaminedtoverifythehighincidenceofHCCinmales.Methods:TumortissuemicroarraywasusedtoexamineBcl-2expressionlevelsin374HCCcasesincluding306malesand68females.Kaplan-Meiermethod,log-ranktest,andCoxproportionalhazardsmodelwereappliedtoinvestigatethepredictivevalueofBcl-2inHCCpatients.Results:ImmunohistochemistryanalysisshowedthatmalepatientswithhigherBcl-2levelshadsignificantlylongermediansurvivaltimeandrecurrencetimethanthosewithlowerlevels.However,nosignificantdifferencesinoutcomeswerefoundbetweendifferentBcl-2levelsinfemalepatients.Whenthemalepatientswerestratifiedintoseveralagepoints,thelevelofBcl-2expressionshowedpoorerpredictiveefficiencyinthe45–49and55–60agegroupsinandropause-agepatientscomparedwithotheragegroups.Bcl-2wasanindependentprognosticfactorforbothoverallsurvival(P<0.0001)andrecurrencetime(P=0.0001)inmalepatients.Afterexcludingmalepatientsinthe45–60agegroup,thepredictiveefficiencywasenhanced(n=147,OS,P=0.0002,TTR,P<0.0001).Conclusions:Bcl-2expressionisanindependentpredictorofsurvivalandrecurrenceinmaleHCC.Bcl-2levelsmayalsoberegulatedbyandrogensorandrogenreceptorsinmaleHCCpatients.Bcl-2levelschangeandexhibitpoorpredictiveefficiencywhenandrogenlevelsvarydramatically(andropauseage).
简介:Objective:Toinvestigatetheeffectoftwoantisenseoligonucleotidesoncellsurviving,bcl-2expressionandapoptosisofleukemiacells.Methods:Theexperimentalassayswereperformedwithcellculture,immunochemistryandflowcytometry.Results:Thetwoantisenseoligodeoxynucleotides,combinedwithVp16orAra-corDNR,wereabletodeclinethesurvivalrateofmyeleukemiccells,downregulatebcl-2geneexpressionandinduceapoptosisofleukemiccellssignificantly,ascomparedwithVp16orAra-corDNRalone.Conclusion:Itispossibleforthetwonewbcl-2antisensestobedevelopedintoclinicaltrialsforleukemiaandtumorwithbcl-2geneoverexpression.
简介:Objective:TostudythedifferencesandsimilaritiesoftheantisensedrugswithdifferentstructuresonthebiologicalfunctionsofK562cells.Methods:Cytotoxiceffectsweremeasuredbyuseofacellviabilityassay.FlowcytometricanalysisandagarosegelelectrophoresisofDNAfragmentationwerealsoperformed.Theexpressionlevelofproteinwasassayedbyimmunofluorescenceusingfluoresceisothiocyanatelabel.Results:PNAtargetingthecodingregionoftheBcl-2messengerRNAcouldeffectivelyinhibitK562cellviability,down-regulatethesynthesisoftheBcl-2proteinandincreasecellapoptosis.By72haftertheBcl-2antisensePNAtreatment,K562cellsshowedmorereductioninthelevelofBcl-2proteincomparedwithcellstreatedwiththeantisenseODN.Aftertreatmentwith10μmol/LofBcl-2antisensePNAorantisenseODNfor72h,apoptoticratesofK562cellswere13.15±1.13and11.72±1.12,respectively.Furthermore,therewassignificantdifferenceinthepercentageofapoptoticcellsbetweenantisensePNAgroupandantisenseODNgroup.Conclusion:TheresultssuggestthatantisensePNAtargetingthecodingregionofBcl-2mRNAhasbetterantisenseeffectsthantheantisenseoligonucleotidesoninducingapoptosisofK562cells.
简介:Objective:TostudytheexpressionofFasandBcl-2proteinsonTlymphocytesubsetsintheperipheralbloodofrelapsingpatientswithcondylomaacuminatum(CA)andhealthycontrols.Methods:Flowcytometry(permeabizationandstainingprocedurewithconjugatedantibodies)wasused.Results:WeobservedthattheexpressionofFasproteinonCD4^+TlymphocytesubsetofCApatientswassignificantlyhigherthanthatofhealthycontrols(P<0.01).Conclusions:IncreasedexpressionofFasproteinonCD4^+Tlymphocytesubsetmaybeacauseofde-creasedpercentageofCD4^+Tlymphocytesubset.ThisinducestheincreasedratioofCD4^+/CD8^+.
简介:Minimalresidualdisease(MRD)playsacausativeroleintumorrecurrenceandestablishmentofeffectiveandsensitiveassessmentofMRDcouldbeveryusefulforstagingandevaluationoftreatmentofdisease.Inthisstudy,weassessedtheusefulnessofhcf-2/JHPCRanalysisonoccultlymphoma...
简介:目的:测定胃黏膜病变组织PCNA、BCL-2和BAX的表达,探讨其在胃黏膜病变过程中的变化规律和所起的作用。方法:用免疫组化染色法检测88例经胃镜和病理确诊的不同胃黏膜病变患者的病变组织中PCNA、BCL-2和BAX的表达,探讨它们之间的关系及变化规律。结果:PCNA从浅表性胃炎→萎缩性胃炎→肠腺化生→异型增生→胃癌中的表达逐渐增强,BCL-2在胃癌中的表达最高,而BAX的表达与BCL-2相反,在浅表性胃炎中表达最强,经相关性分析PCNA与BAX成负相关(r=-0.320,P〈0.01),与BCL-2成正相关(r=-0.430,P〈0.01)。结论:胃黏膜病变从浅表性胃炎→萎缩性胃炎→肠腺化生→异型增生→胃癌的变化过程中,PCNA、BCL-2和BAX表达的异常在其中发挥重要作用。
简介:MitochondrialK+-ATP(mito-KATP)channelsplayanimportantroleincellularfunctionandsurvivalfollowingischemicstress.Thepresentresultsrevealedthatinterventionwithdiazoxide,amito-KATPchannelopener,ledtoanincreaseinBcl-2expressioninthecerebralcortexofratssubjectedtocerebralischemiareperfusioninjury.Inaddition,theinterventionalsoledtoclearimprovementsinneuronalmitochondrialmorphologyandconsciousnesspost-injury.Glibenclamide,amito-KATPchannelblocker,exhibitedtheconverseeffects.Bothdiazoxideandglibenclamideexerteddose-dependenteffects(inparticular,at18mg/kgdiazoxideand25mg/kgglibenclamide).Thesefindingssuggestthatdiazoxideexertsaneuroprotectiveeffectoncerebralischemiareperfusioninjurybyopeningmito-KATPchannelsandupregulatingBcl-2expression.