Vascularstiffnessisanindependentpredictorofcardiovascularmortalityindiabetesandrepresentsan understudied,butpotentiallymodifiableriskfactorfordeathinthelargeandgrowingpopulationofAmerican diabetics.However,themolecularmechanismsunderlyingdiabeticvascularstiffnessareonlyrecentlycoming tolight,andtherapeutictargetsremainelusive. Theapelin-APJsignalingaxisisapotentiallytargetablemolecularpathwaythatisdysregulatedin diabetesandactivationofwhichisassociatedwithdecreasedvascularstiffnessinhumansandmice. Importantly,preliminarydatainapelinknockoutmicesuggeststhatthisdecreasedstiffnessmayoccurinpart throughdecreasedvascularmedialfibrosis.MicroRNA-29b(MiR-29b)protectsagainstmedialfibrosisby translationalrepressionofcollagenandelastintranscripts,anditsexpressionisregulatedbycanonicalsecond messengersofapelin-APJbinding.Therefore,wehypothesizethatdiabetesdecreasesapelin/APJ signaling,leadingtoamiR-29b?dependentalterationincollagenandelastinexpressioninthe vascularmediatocauseincreasedvascularstiffness.
In SpecificAim1, Iwilluseculturedvascularsmoothmusclecellsexposedtoapelinandhyperglycemia aswellasspecificinhibitorsofcanonicalAPJsignalingtoelucidatethespecificmolecularmechanismsby whichapelinincreasesmiR-29bexpressioninthevascularmedia.
In SpecificAim2, Iwilluseamousemodelofdiabetes,theleptinknockout(db/db)mouseaswellas apelinknockoutmicetoassesstheeffectofinvivomodulationofmiR-29bexpressionandapelinondiabetic vascularstiffnessasmeasuredbyexvivopressuremyography.Specifically,IexpecttodemonstratethatmiR- 29badministrationtoapelinKOmicerescuestheirincreaseinvascularstiffness,andthatindb/dbmice,apelin administrationrescuesvascularstiffnessinamiR-29b-dependentmanner.
In SpecificAim3, Iwillexaminetheregulationofthesemolecularactorsinhumandiabetesby measuringaorticexpressionofapelin,APJ,miR-29bandmarkersofvascularmedialfibrosisindiabeticvs non-diabeticpatientswhohaveundergonecoronaryarterybypassgrafting.Thiswillconfirmthattheapelin- APJ-miR-29bpathwayisdownregulatedinhumandiabetes,makingitaviabletherapeutictargettoreduce diabeticvascularstiffness. Theproposedexperimentswillidentifymultipleputativetherapeutictargetsandprovideascaffoldon whichtostudymultiplemolecularpathwaysconvergingonvascularstiffness.Asthisrepresentsoneofthefew targetablediseaseentitiesinwhichinterventioncanpreventmortalityandimprovesymptoms,thisprojecthas thepotentialtocontributegreatlytoourtreatmentofdiabeticcardiovasculardisease.
Diabetesisaprevalentandgrowinghealthissue,anditscardiovascularcomplicationsleadtodeadly outcomes.Vascularstiffnessisamajorriskfactorformorbidityandmortalityinthispopulation,yetno therapiesexisttoaddressit.Here,wewilldefinetheroleofaspecificmolecularpathwaythatprevents vascularstiffnessbutisdeactivatedindiabetes,thusidentifyingpotentialnoveltherapeutictargetstoprevent cardiovasculardeath.
| Parikh, Victoria N; Ashley, Euan A (2017) Next-Generation Sequencing in Cardiovascular Disease: Present Clinical Applications and the Horizon of Precision Medicine. Circulation 135:406-409 |
