the ubiquitin-proteasome system and its role in inflammatory and autoimmune diseases

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1、The Ubiquitin-Proteasome System and Its Role in Inflammatory and Autoimmune DiseasesCellular&MolecularImmunologylview255TheUbiquitin-ProteasomeSystemandItsRoleinInflammatoryandAutoimmuneDiseasesJingsongWang,vandMichaelA.MaldonadoProteindegradationthroughtheubiquitin?-proteasomesystemisthemajorpa

2、thwayofnon?-lysosomalproteolysisofintracellularproteins.Itplaysimportantrolesinavarietyoffundamentalcellularprocessessuchasregulationofcellcycleprogression,division,developmentanddifferentiation,apoptosis,celltrafficking,andmodulationoftheimmuneandinflammatoryresponses.Thecentralelementofthissystemi

3、sthecovalentlinkageofubiquitintotargetedproteins,whichalethenrecognizedbythe26Sproteasome,anadenosinetriphosphate-dependent,multi-catalyticprotease.Damaged,oxidized,ormisfoldedproteinsaswellasregulatoryproteinsthatcontrolmanycriticalcellularfunctionsareamongthetargetsofthisdegradationprocess.Aberrat

4、ionofthissystemleadstothedysregulationofcellularhomeostasisandthedevelopmentofmultiplediseases.Inthisreview,wedescribedthebasicbiochemistryandmolecularbiologyoftheubiquitin-proteasomesystem,anditscomplexroleinthedevelopmentofinflammatoryandantoimmunediseases.Inaddition.therapiesandpotentialtherapeut

5、ictargetsrelatedtotheubiquitin-proteasomesystemarediscussedaswel1.Ce/ular&MolecularImmunology.2006;3(4):255.261.ubiquitin,proteasome,proteindegradation,inflammation,autoimmunediseaseIntroductionThe2004NobelPrizeinChemistrywasawardedtoagroupofscientistsforthediscoveryofthefunctionofubiquitinn.41.

6、Ubiquitinispartoftheubiquitin-proteasomesystem(UPS1matisresponsibleforthedegradationofmorethan80%ofnormalandabnormalintracellularproteins.Attheheartofmissystemisthe26Sproteasome.adynamicmultisubunitproteolyticcomplexwithamolecularweightof700kDthat.ineukaryotes,functionsasthekeyenzymefornon.1ysosomal

7、proteindegradation.Proteasomaldegradationremovesdenatured,misfolded,damagedorimproperlytranslatedproteinsfromcellsandaswellasregulatingthelevelofproteinssuchascyclinsandtranscriptionfactors.Theproductsresultingfromthisenzymaticdegradationhavedifferentsequences,lengthsandbiologicalfunctions(5).ItTran

8、slationalMedicine,WyethResearch,Collegeville,PA19426,USA;DepartmentofMedicine,UniversityofPennsylvania,Philadelphia,PA19104,USA;Correspondingto:Dr.JingsongWang,AssociateDirector,TranslationalMedicine,ClinicalResearchandDevelopment,WyethResearch,500ArcolaRoad,Collegeville,PA19426,USA.Tel:+01-48486583

9、63,Fax:+01-4848651092,Email:jwang8wyeth.corn.ReceivedAug7,2006.AcceptedAug20,2006Copydght2006byTheChineseSocietyofImmunologyhasbeenshownthatthisisahighlyregulated,tightlycontrolled.yetcomplexsystemthatiscentraltonormalcellularhomeostasisincludingcellcycleregulation.DNArepair-sodiumchannelfunction.re

10、gulationofimmuneandinflammatoryresponsesandcellularresponsetostress(6.81.DerangementsoftheUPScanleadtomanydisorders.includingmalignancies,neurodegenerativediseasesandpossiblesystemicautoimmunity(9).BetterunderstandingoftheUPSprocessandidentificationofthecomponentsinvolvedinthedegradationofkeyregulat

11、oryproteinshasleadtothedevelopmentofmechanism.basedtherapeuticsinvariousdiseasesf1012).Agrowingbodyofevidencesuggeststhattargetingtheproteasomalpathwayisanattractiveapproachtotreatinflammatoryandautoimmunediseases(13-15).UbiquitinandubiquitinatiOnUbiquitinisa76.residueproteinthatishighlyevolutionari

12、lyconservedinalleukaryotes(16.17).Selectiveattachmentofubiquitintoproteinsistheinitialsignalfortargetedproteindegradation.Thelinkageofubiquitintothetargetproteinisthroughabranchedisopeptidebondbetweentheubiquitincarboxy1.terminalglycineandaninternallysineonthesubstrate.Additionalubiquitinmoietiesare

13、sequentiallyaddedtoeachothertoformapolyubiquitinchainthatfunctionsastherecognitionsignalforadownstreamproteasomeintheUPS.ModificationoftargetproteinsbyubiquitinoranubiquitinlikeproteinremodelsthesurfaceofVolume3Number4August2006PPI+AMPE1舀一IheUolquiiinPruImc,NyemandItsRolel1.ayAutoi1Ic1uDid0Tar口日捃匕=团

14、-Tl州oStep2Step3pmonlccomplex(2IJSimdarlyIheproteinkinaseCandtyrosmekinasepathwaysareinvolvedinbothIhe.fleaionofbPSsubstratesndphospationElefticientlyrroteasonle20SplYm,afrflncquinatedsubsateslargclednprllteotysisarccognlZenhyproleasomesmecenlralelenlenlofIheUPSInIhepmteasomecclnplcxthecmpltcsfCP)ist

15、hbaclshaped20Scomplex120Spmteasmel(Fi2ure21Itconisisof0urslackedringseachwith7distinctsubunitackedmpofeacholhcrthatresponsibleforthproteolylicaclivit7oftheproteasonleIhclntidentiI_Itcfnngsandw,innerrinsrh【1t2rinhvefm/nownthnction,whereasthe口tingscontainmuhiplecalalytJcSlNIneukaryotes(wooltheeitcsOlltheBril1amchymotrypsiii-likefCTL),wooftheseitctrypsinlikefTUandwoilcaspase-likeEdIIalIkn.wnsyntheticandnatullpmlesonicinhihittrsacln11lhcCTLll(22JbtlmcNUr4Auu21)060专屯Cellular&M0JImmunuklgy19SRegulato

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