Single-cell RNA-sequencing identifies disease-associated oligodendrocytes in male APP NL-G-F and 5XFAD mice
  • Park, Hanseul
  • Cho, Byounggook
  • Kim, Hongwon
  • Saito, Takashi
  • Saido, Takaomi C.
  • ... Kim, Jongpil
  • 외 1명
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초록

Alzheimer's disease (AD) is associated with progressive neuronal degeneration as amyloid-beta (A beta) and tau proteins accumulate in the brain. Glial cells were recently reported to play an important role in the development of AD. However, little is known about the role of oligodendrocytes in AD pathogenesis. Here, we describe a disease-associated subpopulation of oligodendrocytes that is present during progression of AD-like pathology in the male App(NL-G-F) and male 5xFAD AD mouse brains and in postmortem AD human brains using single-cell RNA sequencing analysis. Aberrant Erk1/2 signaling was found to be associated with the activation of disease-associated oligodendrocytes (DAOs) in male App(NL-G-F) mouse brains. Notably, inhibition of Erk1/2 signaling in DAOs rescued impaired axonal myelination and ameliorated A beta-associated pathologies and cognitive decline in the male App(NL-G-F) AD mouse model. Oligodendrocytes have been increasingly shown to be involved in Alzheimer's disease (AD). Here, the authors perform single-cell RNA-sequencing on APP NL-G-F mice and describe a disease-associated oligodendrocyte (DAO) population. They find inhibition of Erk1/2 signaling in DAOs rescues impaired axonal myelination and cognitive decline in an AD mouse model.

키워드

Amyloid Beta ProteinComplement Component C4bCytidine TriphosphateMitogen Activated Protein Kinase 1Protein S100bRnaAmyloid Beta-peptidesAmyloid Beta-protein PrecursorRnaAblimsAmyloid Beta ProteinAnxa5Apolipoprotein ECd59aCd74 AntigenChemokineComplement Component C4bCspg4Cytidine TriphosphateCytokineKallikrein 6Mgst3Mitogen Activated Protein Kinase 1Mitogen Activated Protein Kinase Kinase InhibitorMyelinPlatelet Derived Growth Factor Alpha ReceptorProtein S100bSch 772984Thbs3Transcription Factor Sox6TranscriptomeUnclassified DrugAmyloid Precursor ProteinRnaCellDisease PrevalenceInhibitionMaleNervous System DisorderPathology5xfad MouseAdultAlzheimer DiseaseAnimal CellAnimal ExperimentAnimal ModelAnimal TissueArticleAxonBiochemical AnalysisBrain TissueCell DifferentiationCell SelectionCell SubpopulationControlled StudyCytokine ProductionDifferential Gene ExpressionDisease Associated OligodendrocyteDown RegulationFlow CytometryGene Expression LevelGene LocusHippocampusHumanHuman TissueMapk SignalingMemory DisorderMicrogliaMolecular DynamicsMouseMyelin Forming OligodendrocyteMyelinationNerve Cell DifferentiationNeuropathologyNonhumanOligodendrocyte CultureOligodendrogliaPhenotypeProgeriaProtein ExpressionReference MemoryRisk FactorSingle Cell Rna SeqTranscriptomicsTransmission Electron MicroscopyUpregulationWorking MemoryY-maze TestAnimalDisease ModelGeneticsMetabolismTransgenic MouseAlzheimer DiseaseAmyloid Beta-peptidesAmyloid Beta-protein PrecursorAnimalsDisease Models, AnimalHumansMaleMiceMice, TransgenicOligodendrogliaTRANSGENIC MICEMOUSE MODELSALZHEIMERSMYELINGENEAMYLOIDOSISMICROGLIA
제목
Single-cell RNA-sequencing identifies disease-associated oligodendrocytes in male APP NL-G-F and 5XFAD mice
저자
Park, HanseulCho, ByounggookKim, HongwonSaito, TakashiSaido, Takaomi C.Won, Kyoung-JaeKim, Jongpil
DOI
10.1038/s41467-023-36519-8
발행일
2023-02
유형
Article
저널명
Nature Communications
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