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1、银屑病的生物治疗BiologicaltherapiesforpsoriasisChronicPlaquePsoriasisT-cellmediateddiseaseMenandwomenaffectedequallyGeneticcomponentCircumscribed,raised,redplaquesScaly,itchy,cracking,bleedingModeratetoseverecharacterizedby>10%bodysurfaceareainvolvement,butcanbeupto98%L
2、ife-longdiseasewithnocureConceptbasedon:KruegerJG.JAmAcadDermatol.2002;46:1-23.CytokineproductionKeratinocytehyperproliferationInflammatoryresponseT-cellActivation,Proliferation,andCytokineProductionActivatedAPCT-cellImmunologicSynapseICAMLFA-1MHCTCRCD4/CD8LF
3、A-3CD2CD40CD40LB7CD28ICAMLFA-1CostimulatoryMoleculesCD3CostimulatorySignalsCD11aAntigen-PeptideT-cellActivationSignalsT-cellactivationBiologicalTherapiesofPlaquePsoriasisICAMCD11aLFA-3CD2B7CD28anti-CD11aEfalizumabLFA3-IgAlefaceptCTLA4-IgAbataceptT-cellactivati
4、onInhibitorCytokineInhibitorTNFR-IgEternacetAnti-TNFInfliximabHumanizedmAbIgG1kappahumanframeworkcontainingmurineantibodycomplementarity-determiningregions(CDRs)(MW150kd)GENENTECHBlocksinteractionbetweenLFA-1onT-cellandintracellularadhesionmolecule(ICAM)onAPC,
5、endotheliumandkeratinocytesEfalizumab(Raptiva)CharacteristicsHeavychainLightchainHeavychainCDRLightchainCDRCarbohydratesPhaseIstudy(HU9602)Thisstudyinvestigatedsingleintravenous(IV)doses(0.03,0.1,0.3,0.6,1.0,2.0,3.0or10.0mg/kg)ofefalizumabadministeredinadose-esc
6、alationmannerto31subjectsmoderatetosevereplaquepsoriasis.PhaseIstudyConclusionsTheIVdosageof0.6mg/kg/wkwasthelowestIVdosagethatconsistentlyproducedthemaximalPDeffect.TheSCdosagewasexpectedtobe1.0mg/kg/wkbasedontheestimateofapproximately50%bioavailabilitywiththeS
7、CdosagerelativetoIVadministration.Theaveraget1/2forSCefalizumab1.0mg/kg/wkis5.5daysAlthoughpeakserumconcentrationafterthelastdose(Cmax)washigherforthe2.0mg/kg/wk(30.9μg/mL)thanforthe1.0mg/kg/wkdosage(12.4μg/mL),noadditionalchangesinPDeffectswereobservedatthehigh
8、erdosagesC-EFF-EfalizumabStudy2390:PivotalPhaseIIIEfficacyStudyRandomizationDay0ScreenPrimaryAnalysisWeek12(Day84)Placebo(n=187)Raptiva1mg/kg(n=369)EntrancecriteriaP