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Ageing affects DNA methylation drift and transcriptional cell-to-cell variability in mouse muscle stem cells
by
Commere, Pierre-Henri
, Hernando-Herraez, Irene
, Andrews, Simon
, Jan Bonder, Marc
, Reik, Wolf
, Stubbs, Thomas
, Evano, Brendan
, Tajbakhsh, Shahragim
, Clark, Stephen
in
38
/ 45
/ 45/100
/ 49/23
/ 631/114
/ 631/208/177
/ 631/208/199
/ 631/337/572
/ 631/532/7
/ Aging
/ Animals
/ Cell number
/ Cells, Cultured
/ Cellular Senescence
/ Deoxyribonucleic acid
/ DNA
/ DNA fingerprinting
/ DNA Methylation
/ Drift
/ Epigenesis, Genetic
/ Epigenetics
/ Epigenomics
/ Epigenomics - methods
/ Gene expression
/ Gene Expression Profiling
/ Gene Expression Profiling - methods
/ Gene Ontology
/ Genes
/ Heterogeneity
/ Humanities and Social Sciences
/ Humans
/ Life Sciences
/ Mice, Inbred C57BL
/ Mice, Inbred DBA
/ Mice, Transgenic
/ multidisciplinary
/ Muscles
/ Muscles - cytology
/ Promoter Regions, Genetic
/ Promoter Regions, Genetic - genetics
/ Science
/ Science (multidisciplinary)
/ Single-Cell Analysis
/ Stem cell transplantation
/ Stem Cells
/ Stem Cells - cytology
/ Stem Cells - metabolism
/ Transcriptome
/ Transcriptome - genetics
2019
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Ageing affects DNA methylation drift and transcriptional cell-to-cell variability in mouse muscle stem cells
by
Commere, Pierre-Henri
, Hernando-Herraez, Irene
, Andrews, Simon
, Jan Bonder, Marc
, Reik, Wolf
, Stubbs, Thomas
, Evano, Brendan
, Tajbakhsh, Shahragim
, Clark, Stephen
in
38
/ 45
/ 45/100
/ 49/23
/ 631/114
/ 631/208/177
/ 631/208/199
/ 631/337/572
/ 631/532/7
/ Aging
/ Animals
/ Cell number
/ Cells, Cultured
/ Cellular Senescence
/ Deoxyribonucleic acid
/ DNA
/ DNA fingerprinting
/ DNA Methylation
/ Drift
/ Epigenesis, Genetic
/ Epigenetics
/ Epigenomics
/ Epigenomics - methods
/ Gene expression
/ Gene Expression Profiling
/ Gene Expression Profiling - methods
/ Gene Ontology
/ Genes
/ Heterogeneity
/ Humanities and Social Sciences
/ Humans
/ Life Sciences
/ Mice, Inbred C57BL
/ Mice, Inbred DBA
/ Mice, Transgenic
/ multidisciplinary
/ Muscles
/ Muscles - cytology
/ Promoter Regions, Genetic
/ Promoter Regions, Genetic - genetics
/ Science
/ Science (multidisciplinary)
/ Single-Cell Analysis
/ Stem cell transplantation
/ Stem Cells
/ Stem Cells - cytology
/ Stem Cells - metabolism
/ Transcriptome
/ Transcriptome - genetics
2019
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Ageing affects DNA methylation drift and transcriptional cell-to-cell variability in mouse muscle stem cells
by
Commere, Pierre-Henri
, Hernando-Herraez, Irene
, Andrews, Simon
, Jan Bonder, Marc
, Reik, Wolf
, Stubbs, Thomas
, Evano, Brendan
, Tajbakhsh, Shahragim
, Clark, Stephen
in
38
/ 45
/ 45/100
/ 49/23
/ 631/114
/ 631/208/177
/ 631/208/199
/ 631/337/572
/ 631/532/7
/ Aging
/ Animals
/ Cell number
/ Cells, Cultured
/ Cellular Senescence
/ Deoxyribonucleic acid
/ DNA
/ DNA fingerprinting
/ DNA Methylation
/ Drift
/ Epigenesis, Genetic
/ Epigenetics
/ Epigenomics
/ Epigenomics - methods
/ Gene expression
/ Gene Expression Profiling
/ Gene Expression Profiling - methods
/ Gene Ontology
/ Genes
/ Heterogeneity
/ Humanities and Social Sciences
/ Humans
/ Life Sciences
/ Mice, Inbred C57BL
/ Mice, Inbred DBA
/ Mice, Transgenic
/ multidisciplinary
/ Muscles
/ Muscles - cytology
/ Promoter Regions, Genetic
/ Promoter Regions, Genetic - genetics
/ Science
/ Science (multidisciplinary)
/ Single-Cell Analysis
/ Stem cell transplantation
/ Stem Cells
/ Stem Cells - cytology
/ Stem Cells - metabolism
/ Transcriptome
/ Transcriptome - genetics
2019
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Ageing affects DNA methylation drift and transcriptional cell-to-cell variability in mouse muscle stem cells
Journal Article
Ageing affects DNA methylation drift and transcriptional cell-to-cell variability in mouse muscle stem cells
2019
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Overview
Age-related tissue alterations have been associated with a decline in stem cell number and function. Although increased cell-to-cell variability in transcription or epigenetic marks has been proposed to be a major hallmark of ageing, little is known about the molecular diversity of stem cells during ageing. Here we present a single cell multi-omics study of mouse muscle stem cells, combining single-cell transcriptome and DNA methylome profiling. Aged cells show a global increase of uncoordinated transcriptional heterogeneity biased towards genes regulating cell-niche interactions. We find context-dependent alterations of DNA methylation in aged stem cells. Importantly, promoters with increased methylation heterogeneity are associated with increased transcriptional heterogeneity of the genes they drive. These results indicate that epigenetic drift, by accumulation of stochastic DNA methylation changes in promoters, is associated with the degradation of coherent transcriptional networks during stem cell ageing. Furthermore, our observations also shed light on the mechanisms underlying the DNA methylation clock.
Age-related tissue alterations have been associated with a decline in stem cell number and function. Here the authors report a single cell multi-omics study of mouse muscle stem cells, combining single cell transcriptome and DNA methylome profiling and find that aged cells have a global increase of uncoordinated transcriptional heterogeneity biased towards genes regulating cell-niche interactions.
Publisher
Nature Publishing Group UK,Nature Publishing Group,Nature Portfolio
Subject
/ 45
/ 45/100
/ 49/23
/ 631/114
/ Aging
/ Animals
/ DNA
/ Drift
/ Gene Expression Profiling - methods
/ Genes
/ Humanities and Social Sciences
/ Humans
/ Muscles
/ Promoter Regions, Genetic - genetics
/ Science
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