Klotho and epigenetic regulation of muscle stem cells

McKee, Cynthia

Abstract

Duchennemusculardystrophy(DMD)isalethal,progressive,muscle-wastingdiseasethatinvolvesdefectsin theregenerativecapacityofthepathologicalmuscle.Inrecentyears,expandingknowledgeofepigenetic mechanismsthatinfluencemusclegrowthandregenerationhasshownthatmanipulatingthosemechanisms canbetherapeuticallyuseful.Thefocusofourstudyistodeterminefactorsthataffecttheexpressionof importantepigeneticregulatorsthatcaninfluencegeneexpressioninskeletalmusclestemcells,called satellitecells.WewilltestthenovelhypothesisthattheproteinKlotho(KL)influencesmyogenesisthroughthe epigeneticregulationofsatellitecellactivationanddifferentiation,therebyaffectingmuscleregeneration.We willinvestigatethisthroughthefollowingaims:
Aim1. DeterminewhetherKLinfluencessatellitecellactivationanddifferentiationthroughchangesinhistone methylation.Wewillassaywhetherdown-regulationofspecifichistonedemethylasesinmuscleisasignificant componentofthemechanismthroughwhichKLaffectssatellitecellproliferationandexpressionofmyogenic regulatorygenes.WewillalsoassayforgenesthatexperiencechangesinhistonemethylationatH3K27in musclecellsstimulatedwithKL.
Aim2. DeterminewhethermanipulatingKLexpressionaffectshistonemethylationinsatellitecellsfrommdx mice,amodelforDMD.Wewillassayforchangesinnucleartargetingorexpressionofspecifichistone demethylasesthatresultfromgeneticallyrestoringKLexpressiontodystrophic,mdxmice.Wewillalsoassay forgenesexperiencingchangesinH3K27methylation,causedbyKLtransgeneexpressioninmdxmice WeanticipatethatourfindingswillestablishnovelregulatoryrolesforKL,inwhichtheproteinplaysan epigeneticregulatoryrolethataffectsmyogenesis.Furthermore,theresultsfromthisstudycanprovidethe identityofnewtherapeutictargetstotreatDMDbyimprovingmuscleregeneration.

Public Health Relevance

. Duchennemusculardystrophy(DMD)isalethaldiseasethatcausesprogressivemusclewastingandfailed muscleregeneration.Thisinvestigationwillexamineepigeneticregulatorypathwaysthatpromotemuscle regeneration.Theresultsofthisstudywillexpandunderstandingofpathogenicmechansmsinmuscular dystrophyandexposepotentialtherapeutictargetsforthetreatmentofDMD.

Funding Agency

Agency: National Institute of Health (NIH)
Institute: National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type: Predoctoral Individual National Research Service Award (F31)
Project #: 5F31AR071782-03
Application #: 9997669
Study Section: Special Emphasis Panel (ZRG1)
Program Officer: Boyce, Amanda T

Project Start: 2018-09-01
Project End: 2021-08-31
Budget Start: 2020-09-01
Budget End: 2021-08-31
Support Year: 3
Fiscal Year: 2020
Total Cost
Indirect Cost

Institution

Name: University of California Los Angeles
Department: Physiology
Type: Graduate Schools
DUNS #: 092530369

City: Los Angeles
State: CA
Country: United States
Zip Code: 90095

Related projects


NIH 2020 F31 AR	Klotho and epigenetic regulation of muscle stem cells McKee, Cynthia / University of California Los Angeles
NIH 2019 F31 AR	Klotho and epigenetic regulation of muscle stem cells McKee, Cynthia / University of California Los Angeles
NIH 2018 F31 AR	Klotho and epigenetic regulation of muscle stem cells McKee, Cynthia / University of California Los Angeles

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