The ribonuclease III enzyme Dicer is essential for the processing of micro-RNAs (miRNAs) and small interfering RNAs (siRNAs) from double-stranded RNA precursors. miRNAs and siRNAs regulate chromatin structure, gene transcription, mRNA stability, and translation in a wide range of organisms. To provide a model system to explore the role of Dicer-generated RNAs in the differentiation of mammalian cells in vivo, we have generated a conditional Dicer allele. Deletion of Dicer at an early stage of T cell development compromised the survival of αβ lineage cells, whereas the numbers of γδ-expressing thymocytes were not affected. In developing thymocytes, Dicer was not required for the maintenance of transcriptional silencing at pericentromeric satellite sequences (constitutive heterochromatin), the maintenance of DNA methylation and X chromosome inactivation in female cells (facultative heterochromatin), and the stable shutdown of a developmentally regulated gene (developmentally regulated gene silencing). Most remarkably, given that one third of mammalian mRNAs are putative miRNA targets, Dicer seems to be dispensable for CD4/8 lineage commitment, a process in which epigenetic regulation of lineage choice has been well documented. Thus, although Dicer seems to be critical for the development of the early embryo, it may have limited impact on the implementation of some lineage-specific gene expression programs.
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2 May 2005
Brief Definitive Report|
May 02 2005
T cell lineage choice and differentiation in the absence of the RNase III enzyme Dicer
Bradley S. Cobb,
Bradley S. Cobb
1Lymphocyte Development Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
6Howard Hughes Medical Institute, Department of Microbiology, Immunology, and Molecular Genetics
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Tatyana B. Nesterova,
Tatyana B. Nesterova
2Developmental Epigenetics Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
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Elizabeth Thompson,
Elizabeth Thompson
1Lymphocyte Development Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
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Arnulf Hertweck,
Arnulf Hertweck
1Lymphocyte Development Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
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Eric O'Connor,
Eric O'Connor
3Flow Cytometry Facility, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
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Jonathan Godwin,
Jonathan Godwin
4Transgenics Facility, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
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Christopher B. Wilson,
Christopher B. Wilson
5Department of Immunology, University of Washington, Seattle, WA 98195
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Neil Brockdorff,
Neil Brockdorff
2Developmental Epigenetics Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
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Amanda G. Fisher,
Amanda G. Fisher
1Lymphocyte Development Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
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Stephen T. Smale,
Stephen T. Smale
6Howard Hughes Medical Institute, Department of Microbiology, Immunology, and Molecular Genetics
7Molecular Biology Institute, University of California, Los Angeles, California 90095
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Matthias Merkenschlager
Matthias Merkenschlager
1Lymphocyte Development Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
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Bradley S. Cobb
1Lymphocyte Development Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
6Howard Hughes Medical Institute, Department of Microbiology, Immunology, and Molecular Genetics
Tatyana B. Nesterova
2Developmental Epigenetics Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
Elizabeth Thompson
1Lymphocyte Development Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
Arnulf Hertweck
1Lymphocyte Development Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
Eric O'Connor
3Flow Cytometry Facility, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
Jonathan Godwin
4Transgenics Facility, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
Christopher B. Wilson
5Department of Immunology, University of Washington, Seattle, WA 98195
Neil Brockdorff
2Developmental Epigenetics Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
Amanda G. Fisher
1Lymphocyte Development Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
Stephen T. Smale
6Howard Hughes Medical Institute, Department of Microbiology, Immunology, and Molecular Genetics
7Molecular Biology Institute, University of California, Los Angeles, California 90095
Matthias Merkenschlager
1Lymphocyte Development Group, Medical Research Council Clinical Sciences Centre, Imperial College London, London W12 0NN, England, UK
CORRESPONDENCE Matthias Merkenschlager: [email protected]
Received:
March 17 2005
Accepted:
March 29 2005
Online ISSN: 1540-9538
Print ISSN: 0022-1007
The Rockefeller University Press
2005
J Exp Med (2005) 201 (9): 1367–1373.
Article history
Received:
March 17 2005
Accepted:
March 29 2005
Citation
Bradley S. Cobb, Tatyana B. Nesterova, Elizabeth Thompson, Arnulf Hertweck, Eric O'Connor, Jonathan Godwin, Christopher B. Wilson, Neil Brockdorff, Amanda G. Fisher, Stephen T. Smale, Matthias Merkenschlager; T cell lineage choice and differentiation in the absence of the RNase III enzyme Dicer . J Exp Med 2 May 2005; 201 (9): 1367–1373. doi: https://doi.org/10.1084/jem.20050572
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