298 Current Topics in Microbiology and Immunology Editors R.W.Compans,Atlanta/Georgia M.D.Cooper,Birmingham/Alabama T.Honjo,Kyoto·H.Koprowski,Philadelphia/Pennsylvania F.Melchers,Basel·M.B.A.Oldstone,LaJolla/California S.Olsnes,Oslo·M.Potter,Bethesda/Maryland P.K.Vogt,LaJolla/California·H.Wagner,Munich E. Vivier and M. Colonna (Eds.) Immunobiology of Natural Killer Cell Receptors With27Figuresand8Tables 123 EricVivier,DVM,PhD. LaboratoryofNKCellsandInnateImmunity Centred’ImmunologiedeMarseille-Luminy(CIML) CNRS-INSERM-UniversitédelaMéditerranée CampusdeLuminy,Case906 13288MarseilleCedex09 France e-mail:[email protected] MarcoColonna,M.D. DepartmentofPathologyandImmunology WashingtonUniversitySchoolofMedicine WestBuilding,Rooms4724,Box8118 660SouthEuclidAve St.Louis,MO63110 USA e-mail:[email protected] Coverillustration:NaturalKiller(NK)cellactivationresultsfromadynamicequilibriumbetween complementaryandsometimeantagonistforces,suchasthatinitiatedbyactivatingreceptors recognizing stress-induced self (e.g. NKG2D ligands) and inhibitory receptors recognizing constitutively-expressedself(e.g.MHCclassImolecules). LibraryofCongressCatalogNumber72-152360 ISSN 0070-217X ISBN-10 3-540-26083-8 SpringerBerlinHeidelbergNewYork ISBN-13 978-3-540-26083-7 SpringerBerlinHeidelbergNewYork Thisworkissubjecttocopyright.Allrightsreserved,whetherthewholeorpartofthematerial isconcerned,specificallytherightsoftranslation,reprinting,reuseofillustrations,recitation, broadcasting,reproductiononmicrofilmorinanyotherway,andstorageindatabanks.Dupli- cationofthispublicationorpartsthereofispermittedonlyundertheprovisionsoftheGerman CopyrightLawofSeptember,9,1965,initscurrentversion,andpermissionforusemustal- waysbeobtainedfromSpringer-Verlag.ViolationsareliableforprosecutionundertheGerman CopyrightLaw. 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Editor:SimonRallison,Heidelberg Deskeditor:AnneClauss,Heidelberg Productioneditor:NadjaKroke,Leipzig Coverdesign:design&productionGmbH,Heidelberg Typesetting:LE-TEXJelonek,Schmidt&VöcklerGbR,Leipzig Printedonacid-freepaper SPIN11332404 27/3150/YL – 5 4 3 2 1 0 ListofContents StrategiesofNaturalKillerCellRecognitionandSignaling ................ 1 C.A.Stewart,E.Vivier,andM.Colonna SignalTransductioninNaturalKillerCells ........................... 23 A.W.MacFarlaneIVandK.S.Campbell TranscriptionalRegulationofNKCellReceptors ....................... 59 S.K.Anderson ExtendingMissing-Self?FunctionalInteractionsBetweenLectin-like Nkrp1ReceptorsonNKCellswithLectin-likeLigands................... 77 B.F.M.PlougastelandW.M.Yokoyama TheCD2FamilyofNaturalKillerCellReceptors ....................... 91 M.E.McNerneyandV.Kumar ImmunobiologyofHumanNKG2DandItsLigands .....................121 S.González,V.Groh,andT.Spies NKG2Receptor-MediatedRegulationofEffectorCTLFunctions intheHumanTissueMicroenvironment.............................139 B.JabriandB.Meresse DendriticCell–NKCellCross-Talk:RegulationandPhysiopathology.. .......157 L.Zitvogel,M.Terme,C.Borg,andG.Trinchieri NKCellActivatingReceptorsandTumorRecognitioninHumans ...........175 C.Bottino,L.Moretta,andA.Moretta NKCellRecognitionofMouseCytomegalovirus-InfectedCells.............183 S.M.VidalandL.L.Lanier NKCellReceptorsInvolvedintheResponsetoHuman CytomegalovirusInfection ......................................207 M.Gumá,A.Angulo,andM.López-Botet VI ListofContents TheImpactofVariationattheKIRGeneClusteronHumanDisease .........225 M.CarringtonandM.P.Martin NKCellsinAutoimmuneDisease..................................259 S.Johansson,H.Hall,L.Berg,andP.Höglund SubjectIndex................................................279 ListofContributors (Addressesstatedatthebeginningofrespectivechapters) Anderson,S.K. 59 Lanier,L.L. 183 Angulo,A. 207 López-Botet,M. 207 MacFarlaneIV,A.W. 23 Berg,L. 259 Martin,M.P. 225 Borg,C. 157 McNerney,M.E. 91 Bottino,C. 175 Meresse,B. 139 Moretta,A. 175 Campbell,K.S. 23 Moretta,L. 175 Carrington,M. 225 Colonna,M. 1 Plougastel,B.F.M. 77 González,S. 121 Spies,T. 121 Groh,V. 121 Stewart,C.A. 1 Gumá,M. 207 Terme,M. 157 Höglund,P. 259 Trinchieri,G. 157 Hall,H. 259 Vidal,S.M. 183 Vivier,E. 1 Jabri,B. 139 Johansson,S. 259 Yokoyama,W.M. 77 Kumar,V. 91 Zitvogel,L. 157 CTMI(2006)298:1–21 (cid:1)c Springer-VerlagBerlinHeidelberg2006 StrategiesofNaturalKillerCellRecognition andSignaling C.A.Stewart1((cid:1))·E.Vivier1·M.Colonna2 1LabofNKCellsandInnateImmunity,Centred’ImmunologiedeMarseille-Luminy, INSERM-CNRS-Univ.Méditerranée,CampusdeLuminy, 13288Marseillecedex09, France [email protected] 2DepartmentofPathologyandImmunology,WashingtonUniversitySchoolof Medicine,St.Louis,MO63110,USA 1 Introduction ........................................... 2 2 ThemesofNKCellRecognition .............................. 2 3 InhibitoryRecognitionandSignaling ......................... 3 3.1 InhibitoryReceptorsforMHCClassI .......................... 3 3.2 InhibitoryReceptorsforNon-MHCLigands ..................... 6 4 ActivatingRecognitionandSignaling ......................... 6 4.1 SomeITAM-BasedReceptors................................ 6 4.2 NKG2D ............................................... 7 4.3 ActivatingHomologsofInhibitoryMHCClassIReceptors ........... 7 5 TheNKCellActivationCascade:FromSurfaceTriggerstoEffectorFunction 8 6 ComplexitiesinNKCellActivation ........................... 10 6.1 ConsequencesofITIMPhosphorylation ........................ 10 6.2 2B4InhibitionandActivation ............................... 10 6.3 RolesofAdhesion........................................ 11 6.4 CytotoxicityandCytokineResponses .......................... 12 7 AChallengefortheFuture:UnderstandingtheIntegrationofSignals byNKCells ............................................ 13 References.................................................. 14 Abstract Theparticipationofnaturalkiller(NK)cellsinmultipleaspectsofinnate andadaptiveimmuneresponsesissupportedbythewidearrayofstimulatoryand inhibitoryreceptorstheybear.Herewereviewthereceptor-ligandinteractionsand subsequentsignalingeventsthatculminateinNKeffectorresponses.Whereassome receptor-ligandinteractionsresultinactivationofbothNKcytotoxicityandcytokine 2 C.A.Stewartetal. production,othershavemoresubtleeffects,selectivelyactivatingonlyonepathway orhavingdistinctcontext-dependenteffects.Recentapproachesofferwaystounravel howtheintegrationofcomplexsignalingnetworksdirectstheNKresponse. 1 Introduction Natural killer (NK) cells are large granular lymphocytes of the innate im- mune system. They are widespread throughout the body, being present in both lymphoid organs and nonlymphoid peripheral tissues (Cooper et al. 2004;FerlazzoandMunz2004).NKcellsareinvolvedindirectinnateimmune reactionsagainstviruses,bacteria,parasites,andothertriggersofpathology, suchasmalignanttransformation,allofwhichcausestressinaffectedcells (Morettaetal.2002;Raulet2004).Importantly,NKcellsalsolinktheinnate andadaptiveimmuneresponses,contributingtotheinitiationofadaptiveim- muneresponses(seechapterbyZitvogeletal.,thisvolume)(Martin-Fontecha γ et al. 2004) and executing adaptive responses with the CD16 Fc RIIIA im- munoglobulinFcreceptor.Suchresponsesaremediatedthroughtwomajor effectorfunctions,thedirectcytolysisoftargetcellsandtheproductionofcy- tokinesandchemokines.Wefocushereonthenatureofrecognitioneventsby NKcellsandaddresshowtheseeventsareintegratedtotriggerthesedistinct andgradedeffectorfunctions. 2 ThemesofNKCellRecognition The dissection of NK cell innate recognition strategies was initiated by the discoverythatNKcellcytotoxicityinverselycorrelateswiththelevelofmajor histocompatibility complex (MHC)class Iexpression on target cells (Karre etal.1986).Themissingselfhypothesiselegantlyprovidedanexplanationfor this phenomenon and led to the discovery of multiple inhibitory receptors thatblockactivatingsignalsbyrecruitmentofproteintyrosinephosphatases totheirintracytoplasmicimmunoreceptortyrosine-basedinhibitionmotifs (ITIMs)(Long1999;VivierandDaëron1997).Opposingthisinhibitorysig- naling,innatestimulatoryrecognitionbyNKcellscanbeclassifiedinthree generalmodes:recognitionofconstitutivelyexpressedselfmolecules,recog- nitionofmotifsupregulatedbystressedcells,anddirectrecognitionofinfec- tiouspathogencomponents(Raulet2004;VivierandMalissen2005).Together, StrategiesofNaturalKillerCellRecognition andSignaling 3 thenumerous receptors carrying out these functions allow NK cells to dis- criminatebetweentargetandnon-targetcells(Fig.1)(CerwenkaandLanier 2001;VilchesandParham2002;VivierandBiron2002;Yokoyama1998).Only aminorityofthesereceptors,suchasthenaturalcytotoxicityreceptors(NCR), aretrulyNKcellspecific,withmanybeingfoundonotherhematopoieticcells. Thequestionofhowallthesignalsareintegratedfrommultiple,redundant andopposing,simultaneouslyengagedpathwaystoculminateingradedNK cellresponses,thatis,cytotoxicityand/orcytokineproduction,servestoillus- tratethecomplexanddynamicallybalancednatureofcellactivation(Lanier 2003;Vivieretal.2004). 3 InhibitoryRecognitionandSignaling 3.1 InhibitoryReceptorsforMHCClassI Multiple families of receptors in mouse and human recognize MHC class I products and transmit inhibitory signals when engaged. CD94/NKG2 receptorsareheterodimersofC-typelectintypeIItransmembraneproteins that recognize the nonclassical MHC class I molecules HLA-E (human leukocyteantigen-E,inhuman)andQa-1b (inmouse)(Borregoetal.1998; Braud et al. 1998; Lee et al. 1998; Vance et al. 1998). Of the NKG2 family members that associate with CD94 (including NKG2A, C, and E), NKG2A contains ITIMs in its cytoplasmic domain conferring inhibitory function. Recognition of HLA-E or Qa-1b by CD94/NKG2 requires the presence of peptidesinthepeptidebindinggroovesoftheseclassImolecules.Manyof thesepeptidesarederivedfromtheleadersequencesofclassicalMHCclass Imolecules(Braudetal.1997;Kraftetal.2000),thusmakingCD94/NKG2A a sensor of active MHC class I biosynthesis and presentation. CD94/NKG2 is unique in both its high evolutionary conservation and its means of recognizingclassicalMHCclassIasa“proxy”sensor. MembersofotherNKcellMHCclassIreceptorfamiliesdirectlybindto classicalMHCclassImolecules.Inthemouseandrat,NKcellrecognitionof subsetsofMHCclassIallotypesismediatedbymembersoftheLy49family ofC-typelectintypeIItransmembraneproteins.Incontrast,humanNKcells useimmunoglobulindomain-containingtypeItransmembraneproteinsfor thesamefunction.Theimmunoglobulin-liketranscript2(ILT2,orLIR1)re- ceptorrecognizesabroadrangeofbothclassicalandnonclassicalMHCclass I molecules (Chapman et al. 1999; Colonna et al. 1997), whereas members