Abstract

Reactiveoxygenspecies(ROS)areemergingascriticalsecondmessengersinmanysignalingpathways relatedtohealthanddisease.Whilemuchprogresshasbeenmadeinunderstandingthemechanismsby whichROSlevelsareregulatedinsidecells,lessisknownaboutthemolecularsignalingeventsthatoccur downstreamofROSgeneration.Agrowingbodyofevidencesuggeststhatproteinkinasesaredirectly regulatedbyROSmodification.Forinstance,thereversibleoxidationofspecificCysresiduesinredox- sensitivekinaseshasbeenshowntoinfluencetheiractivity(eitherpositivelyornegatively),subcellular localization,andprotein-proteininteractions.Inmanycases,themodifiedCysintheaffectedkinaseis conservedamongothermembersinthesamekinasefamily.Thisraisesthepossibilitythatreversibleoxidation maybeageneralmeansofregulatingkinasefunctioninsidecells.Toexplorethispossibilityfurther,we recentlyusedfunctionalproteinmicroarraystoexaminetheimpactofoxidationontheglobalsubstrate selectionofaseriesofAGCandCMCGkinasefamilymembers.ThesestudiessuggestthatH2O2-dependent oxidationshiftsthesubstratepreferenceofmanykinases,leadingtodistinctsubstrateprofilesintheoxidized andreducedstates.Interestingly,inmostcases,bothincreasesanddecreasesinsubstratephosphorylation wereobserved.Asaconsequence,reversibleoxidationmayplayanimportantroleincontrollingthesignaling specificityofredox-sensitivekinasesincells.Toinvestigatethesequestionsfurther,wepropose1)toexamine themolecularmechanismsunderlyingtheH2O2-inducedshiftsinkinasesubstrateselection(Aims1&2)and 2)tobegintoexplorethefunctionalconsequencesofredoxmodificationonkinase-dependentsignaling processesinsidethecell(Aim3).Duringthesestudies,wewillfocusontworepresentativeAGCandCMGC familymembers,namelyPKAandERK2.Notonlywillthisprovidenewinsightsintotheredoxregulationof theseimportantkinases,butitwillalsolayafoundationfortheanalysisofotherredoxsensitivekinases identifiedinthemicroarrayexperiments.Together,thesestudieswillofferuniqueinsightsintoROS-mediated regulationofkinasefunctionandprovidethefoundationforfuturestudiesintocrosstalkbetweenROS-and phosphorylation-dependentsignalingpathwaysinphysiologicalandpathologicalstates.

Public Health Relevance

Intheproposedproject,weplanto1)investigatethebiochemicalmechanismsunderlyingoxidation- inducedshiftsinproteinkinasesubstrateselectionand2)begintoexplorethefunctionalconsequencesof redoxmodificationonkinase-dependentsignalingprocessesinsidecells.Duringthesestudies,wewillfocus onPKAa?andERK2asrepresentativemembersoftheAGCandCMGCkinasefamilies.Notonlywillthe proposedstudiesprovidenewinsightsintotheredoxregulationoftheseimportantkinases,buttheywillalso layafoundationfortheanalysisofotherredox-sensitivekinases.Together,thesestudieswillhelpidentify pointsofsignalintegrationbetweenROS-andphosphorylation-dependentpathways.Theywillalso complementexistingmodelsofpathologicaloxidativestressandprovidenewopportunitiesfortargeted antioxidanttherapeuticsformanydiseases(e.g.,cancer,diabetesandcardiovasculardisease).

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Enhancement Award (SC1)
Project #
1SC1GM130545-01
Application #
9633575
Study Section
Special Emphasis Panel (ZGM1)
Program Officer
Barski, Oleg
Project Start
2018-09-10
Project End
2022-07-31
Budget Start
2018-09-10
Budget End
2019-07-31
Support Year
1
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
North Carolina Agri & Tech State University
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
071576482
City
Greensboro
State
NC
Country
United States
Zip Code
27411