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Pim-3基因对暴发性肝衰竭的肝保护效应研究的开题报告Title:ThehepatoprotectiveeffectofPim-3geneonacuteliverfailureBackgroundandsignificance:Acuteliverfailure(ALF)isalife-threateningconditioncharacterizedbyrapidandseverehepaticdysfunction.Despiterecentadvancesinlivertransplantationandsupportivecare,themortalityrateofALFremainshigh.Therefore,itisurgenttoidentifynewtherapeutictargetsandmolecularmechanismstoimprovetheoutcomesofpatientswithALF.Pim-3isaserine/threoninekinasethathasbeenshowntoplayacriticalroleincellproliferation,survival,anddifferentiation.RecentstudieshavesuggestedthatPim-3hasaprotectiveeffectonliverinjuryinducedbyvariousinsults,suchasischemia-reperfusion,acetaminophenoverdose,andalcoholexposure.However,theroleofPim-3inALFisnotwellunderstood.Researchquestionandhypotheses:ThisstudyaimstoinvestigatethehepatoprotectiveeffectofPim-3geneonacuteliverfailureandexploretheunderlyingmechanisms.WehypothesizethatoverexpressionofPim-3geneinhepatocytescanattenuateliverinjuryinducedbydifferentALFmodelsandimprovethesurvivalrateofmicewithALF.WespeculatethattheprotectiveeffectofPim-3maybemediatedbyinhibitingapoptosis,activatingautophagy,andregulatingtheinflammationresponseinALF.Materialsandmethods:1.Animalmodels:Wewilluseamousemodelofacetaminophen-inducedALFandamodeloflipopolysaccharide/d-galactosamine-inducedALFinthisstudy.2.ConstructionandvalidationofPim-3overexpressionplasmids:Thefull-lengthPim-3cDNAwillbeclonedintothelentiviralvectorpLVX-EF1α-IRES-PurotogeneratethePim-3overexpressionplasmids.TheplasmidswillbeverifiedbyDNAsequencing,andtheexpressionofPim-3proteinwillbeconfirmedbyWesternblotanalysis.3.Lentivirus-mediatedgenetransfer:ThePim-3overexpressionplasmidswillbetransfectedintoprimaryhepatocytesusinglentiviralvec