中图分类号：R542.2 文献标识码：A文章编号：1006-1959(2025)09-0008-06

    DOI：10.3969/j.issn.1006-1959.2025.09.002

    Abstract：ObjectiveToinvestigatethepathogenicmechanismofFKTNgene mutationindilatedcardiomyopathy.MethodsTeGSE13828gene expressionproflrelatedtFKasdwladedfroteGenExpressonObsdatabaseandedierentialexpresionofKgene mutationmyocadaltiendalardalisueasaldTapRpacgessedtisplatfretiallexpd intheFKTgeneutantmyocardialtissendfurtereichmentaalysisofthdiferentillyexpressedgneswasperfodtfindte enrchentpathwaysProteninteractionetwokaalysisassedtofindtheeypathayproteisinthKeneutantmyocadaltisuead tofiditspathogenicmechanismandtherapeutictargetsResultsoifoaticsaalysisofFKTgneshowedtatcomparedwithtehealty controlgroup636ieetialypresentiutatioofcglatedde dow-regulatedAogtegatdGOalisdtatitasainlyentratedinatospodetaceai colgenfiberproiferationKEGGpathwayanalysisfoundtatteyweremainlyeicedinteinteractionofyokineytokinepto interleuki-igaingathactoiltainaligtaaligtad matrixeceteacteactiokaldatdC; regulatedgeesaldatleraediaspadalactdpmc microtubuleandproteinglycosylatioKEGGpathwayaalysisfoundthattheyweremainlycocentratedinmyocardialontractioilated cardiomyopathyandcalciumsignalingpathway.ProteininteractionnetworkanalysisfoundthatthekeynodegeneswereAsbl5andEfcab2. ConclusionThepathogenesisofmicewithFKTNmutation-relatedDCMmayberelatedtointracardiaccalciumhomeostasis ......