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Histone demethylases UTX and JMJD3 are required for NKT cell development in mice
Histone demethylases UTX and JMJD3 are required for NKT cell development in mice
by Northrup, Daniel , Placek, Katarzyna , Zhu, Jinfang , Pohl, Lance R. , Zhao, Keji , Yagi, Ryoji , Wang, Chaochen , Wang, Rongfu , Cui, Kairong , Proctor, William R. , Ge, Kai
in Biomedical and Life Sciences / Bone marrow / CD4 antigen / Cell Biology / Cell cycle / Clonal deletion / Concanavalin A / Data processing / Developmental Block / DNA methylation / Double Positive / Enzymes / Epigenetics / Flow cytometry / Gene expression / Genomes / H3K27 Methylation / Hepatitis / Hepatocytes / iNKT Cell / Life Sciences / Lipids / Liver / Lymphocytes / Lymphocytes T / Microbiology / Natural killer cells / Neurobiology / Proteins / Proteomics / Ribonucleic acid / RNA / Rodents / Stem Cells / T cell receptors / Transcription factors / Wild Type CD45
2017
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Histone demethylases UTX and JMJD3 are required for NKT cell development in mice
by Northrup, Daniel , Placek, Katarzyna , Zhu, Jinfang , Pohl, Lance R. , Zhao, Keji , Yagi, Ryoji , Wang, Chaochen , Wang, Rongfu , Cui, Kairong , Proctor, William R. , Ge, Kai
in Biomedical and Life Sciences / Bone marrow / CD4 antigen / Cell Biology / Cell cycle / Clonal deletion / Concanavalin A / Data processing / Developmental Block / DNA methylation / Double Positive / Enzymes / Epigenetics / Flow cytometry / Gene expression / Genomes / H3K27 Methylation / Hepatitis / Hepatocytes / iNKT Cell / Life Sciences / Lipids / Liver / Lymphocytes / Lymphocytes T / Microbiology / Natural killer cells / Neurobiology / Proteins / Proteomics / Ribonucleic acid / RNA / Rodents / Stem Cells / T cell receptors / Transcription factors / Wild Type CD45
2017
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Histone demethylases UTX and JMJD3 are required for NKT cell development in mice
Histone demethylases UTX and JMJD3 are required for NKT cell development in mice
by Northrup, Daniel , Placek, Katarzyna , Zhu, Jinfang , Pohl, Lance R. , Zhao, Keji , Yagi, Ryoji , Wang, Chaochen , Wang, Rongfu , Cui, Kairong , Proctor, William R. , Ge, Kai
in Biomedical and Life Sciences / Bone marrow / CD4 antigen / Cell Biology / Cell cycle / Clonal deletion / Concanavalin A / Data processing / Developmental Block / DNA methylation / Double Positive / Enzymes / Epigenetics / Flow cytometry / Gene expression / Genomes / H3K27 Methylation / Hepatitis / Hepatocytes / iNKT Cell / Life Sciences / Lipids / Liver / Lymphocytes / Lymphocytes T / Microbiology / Natural killer cells / Neurobiology / Proteins / Proteomics / Ribonucleic acid / RNA / Rodents / Stem Cells / T cell receptors / Transcription factors / Wild Type CD45
2017

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Histone demethylases UTX and JMJD3 are required for NKT cell development in mice
Histone demethylases UTX and JMJD3 are required for NKT cell development in mice
Journal Article

Histone demethylases UTX and JMJD3 are required for NKT cell development in mice

Northrup, Daniel,
Placek, Katarzyna,
Zhu, Jinfang,
Pohl, Lance R.,
Zhao, Keji,
Yagi, Ryoji,
Wang, Chaochen,
Wang, Rongfu,
Cui, Kairong,
Proctor, William R.,
Ge, Kai
2017
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Overview
Background Natural killer (NK)T cells and conventional T cells share phenotypic characteristic however they differ in transcription factor requirements and functional properties. The role of histone modifying enzymes in conventional T cell development has been extensively studied, little is known about the function of enzymes regulating histone methylation in NKT cells. Results We show that conditional deletion of histone demethylases UTX and JMJD3 by CD4-Cre leads to near complete loss of liver NKT cells, while conventional T cells are less affected. Loss of NKT cells is cell intrinsic and not due to an insufficient selection environment. The absence of NKT cells in UTX/JMJD3-deficient mice protects mice from concanavalin A‐induced liver injury, a model of NKT‐mediated hepatitis. GO‐analysis of RNA-seq data indicates that cell cycle genes are downregulated in UTX/JMJD3-deleted NKT progenitors, and suggest that failed expansion may account for some of the cellular deficiency. The phenotype appears to be demethylase‐dependent, because UTY, a homolog of UTX that lacks catalytic function, is not sufficient to restore their development and removal of H3K27me3 by deletion of EZH2 partially rescues the defect. Conclusions NKT cell development and gene expression is sensitive to proper regulation of H3K27 methylation. The H3K27me3 demethylase enzymes, in particular UTX, promote NKT cell development, and are required for effective NKT function.
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Publisher
BioMed Central,Springer Nature B.V,BMC
Subject

Biomedical and Life Sciences

/ Bone marrow

/ CD4 antigen

/ Cell Biology

/ Cell cycle

/ Clonal deletion

/ Concanavalin A

/ Data processing

/ Developmental Block

/ DNA methylation

/ Double Positive

/ Enzymes

/ Epigenetics

/ Flow cytometry

/ Gene expression

/ Genomes

/ H3K27 Methylation

/ Hepatitis

/ Hepatocytes

/ iNKT Cell

/ Life Sciences

/ Lipids

/ Liver

/ Lymphocytes

/ Lymphocytes T

/ Microbiology

/ Natural killer cells

/ Neurobiology

/ Proteins

/ Proteomics

/ Ribonucleic acid

/ RNA

/ Rodents

/ Stem Cells

/ T cell receptors

/ Transcription factors

/ Wild Type CD45

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