Epigenetic inheritance of cell differentiation status

Epigenetic modifications influence gene expression pattern and provide a unique signature of a cell differentiation status. Without external stimuli or signalling events, this cell identity remains stable and unlikely to change over many cell divisions. The epigenetic signature of a particular cell...

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Published inCell cycle (Georgetown, Tex.) Vol. 7; no. 9; pp. 1173 - 1177
Main Authors Ng, Ray K., Gurdon, John B.
Format Journal Article
LanguageEnglish
Published United States Taylor & Francis 01.05.2008
Subjects
Animals
Binding
Biology
Bioscience
Calcium
Cancer
Cell
Cell Differentiation - genetics
Cell Lineage - genetics
Chromatin Assembly and Disassembly - genetics
Cycle
Epigenesis, Genetic - genetics
Gene Expression Regulation - genetics
Histones - genetics
Humans
Inheritance Patterns - genetics
Landes
Models, Biological
Nucleosomes - genetics
Organogenesis
Proteins
Online AccessGet full text

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Abstract Epigenetic modifications influence gene expression pattern and provide a unique signature of a cell differentiation status. Without external stimuli or signalling events, this cell identity remains stable and unlikely to change over many cell divisions. The epigenetic signature of a particular cell fate therefore needs to be replicated faithfully in daughter cells; otherwise a cell lineage cannot be maintained. However, the mechanism of transmission of cellular memory from mother to daughter cells remains unclear. It has been suggested that the inheritance of an active or silent gene state involves different kinds of epigenetic mechanisms, e.g. DNA methylation, histone modifications, replacement of histone variants, Polycomb group (PcG) and Trithorax group (TrxG) proteins. Emerging evidence supports the role of histone variant H3.3 in maintaining an active gene status and in remodelling nucleosomal composition. Here we discuss some recent findings on the propagation of epigenetic memory and propose a model for the inheritance of an active gene state through the interaction of H3.3 with other epigenetic components.
AbstractList Epigenetic modifications influence gene expression pattern and provide a unique signature of a cell differentiation status. Without external stimuli or signalling events, this cell identity remains stable and unlikely to change over many cell divisions. The epigenetic signature of a particular cell fate therefore needs to be replicated faithfully in daughter cells; otherwise a cell lineage cannot be maintained. However, the mechanism of transmission of cellular memory from mother to daughter cells remains unclear. It has been suggested that the inheritance of an active or silent gene state involves different kinds of epigenetic mechanisms, e.g. DNA methylation, histone modifications, replacement of histone variants, Polycomb group (PcG) and Trithorax group (TrxG) proteins. Emerging evidence supports the role of histone variant H3.3 in maintaining an active gene status and in remodelling nucleosomal composition. Here we discuss some recent findings on the propagation of epigenetic memory and propose a model for the inheritance of an active gene state through the interaction of H3.3 with other epigenetic components.
Author Ng, Ray K.
Gurdon, John B.
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BackLink https://www.ncbi.nlm.nih.gov/pubmed/18418041$$D View this record in MEDLINE/PubMed
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Snippet Epigenetic modifications influence gene expression pattern and provide a unique signature of a cell differentiation status. Without external stimuli or...
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SubjectTerms Animals
Binding
Biology
Bioscience
Calcium
Cancer
Cell
Cell Differentiation - genetics
Cell Lineage - genetics
Chromatin Assembly and Disassembly - genetics
Cycle
Epigenesis, Genetic - genetics
Gene Expression Regulation - genetics
Histones - genetics
Humans
Inheritance Patterns - genetics
Landes
Models, Biological
Nucleosomes - genetics
Organogenesis
Proteins
Title Epigenetic inheritance of cell differentiation status
URI https://www.tandfonline.com/doi/abs/10.4161/cc.7.9.5791
http://www.landesbioscience.com/journals/cc/article/5791/
https://www.ncbi.nlm.nih.gov/pubmed/18418041
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Volume 7
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