RNA-mediated epigenetic heredity requires the cytosine methyltransferase Dnmt2.

RNA-mediated transmission of phenotypes is an important way to explain non-Mendelian heredity. We have previously shown that small non-coding RNAs can induce hereditary epigenetic variations in mice and act as the transgenerational signalling molecules. Two prominent examples for these paramutations...

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Main Authors: Jafar Kiani, Valérie Grandjean, Reinhard Liebers, Francesca Tuorto, Hossein Ghanbarian, Frank Lyko, François Cuzin, Minoo Rassoulzadegan
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-05-01
Series:PLoS Genetics
Online Access:http://europepmc.org/articles/PMC3662642?pdf=render
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spelling doaj-24a14fbbd6394eb8a6c6c8f23599bebd2020-11-25T01:26:49ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042013-05-0195e100349810.1371/journal.pgen.1003498RNA-mediated epigenetic heredity requires the cytosine methyltransferase Dnmt2.Jafar KianiValérie GrandjeanReinhard LiebersFrancesca TuortoHossein GhanbarianFrank LykoFrançois CuzinMinoo RassoulzadeganRNA-mediated transmission of phenotypes is an important way to explain non-Mendelian heredity. We have previously shown that small non-coding RNAs can induce hereditary epigenetic variations in mice and act as the transgenerational signalling molecules. Two prominent examples for these paramutations include the epigenetic modulation of the Kit gene, resulting in altered fur coloration, and the modulation of the Sox9 gene, resulting in an overgrowth phenotype. We now report that expression of the Dnmt2 RNA methyltransferase is required for the establishment and hereditary maintenance of both paramutations. Our data show that the Kit paramutant phenotype was not transmitted to the progeny of Dnmt2(-/-) mice and that the Sox9 paramutation was also not established in Dnmt2(-/-) embryos. Similarly, RNA from Dnmt2-negative Kit heterozygotes did not induce the paramutant phenotype when microinjected into Dnmt2-deficient fertilized eggs and microinjection of the miR-124 microRNA failed to induce the characteristic giant phenotype. In agreement with an RNA-mediated mechanism of inheritance, no change was observed in the DNA methylation profiles of the Kit locus between the wild-type and paramutant mice. RNA bisulfite sequencing confirmed Dnmt2-dependent tRNA methylation in mouse sperm and also indicated Dnmt2-dependent cytosine methylation in Kit RNA in paramutant embryos. Together, these findings uncover a novel function of Dnmt2 in RNA-mediated epigenetic heredity.http://europepmc.org/articles/PMC3662642?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Jafar Kiani
Valérie Grandjean
Reinhard Liebers
Francesca Tuorto
Hossein Ghanbarian
Frank Lyko
François Cuzin
Minoo Rassoulzadegan
spellingShingle Jafar Kiani
Valérie Grandjean
Reinhard Liebers
Francesca Tuorto
Hossein Ghanbarian
Frank Lyko
François Cuzin
Minoo Rassoulzadegan
RNA-mediated epigenetic heredity requires the cytosine methyltransferase Dnmt2.
PLoS Genetics
author_facet Jafar Kiani
Valérie Grandjean
Reinhard Liebers
Francesca Tuorto
Hossein Ghanbarian
Frank Lyko
François Cuzin
Minoo Rassoulzadegan
author_sort Jafar Kiani
title RNA-mediated epigenetic heredity requires the cytosine methyltransferase Dnmt2.
title_short RNA-mediated epigenetic heredity requires the cytosine methyltransferase Dnmt2.
title_full RNA-mediated epigenetic heredity requires the cytosine methyltransferase Dnmt2.
title_fullStr RNA-mediated epigenetic heredity requires the cytosine methyltransferase Dnmt2.
title_full_unstemmed RNA-mediated epigenetic heredity requires the cytosine methyltransferase Dnmt2.
title_sort rna-mediated epigenetic heredity requires the cytosine methyltransferase dnmt2.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2013-05-01
description RNA-mediated transmission of phenotypes is an important way to explain non-Mendelian heredity. We have previously shown that small non-coding RNAs can induce hereditary epigenetic variations in mice and act as the transgenerational signalling molecules. Two prominent examples for these paramutations include the epigenetic modulation of the Kit gene, resulting in altered fur coloration, and the modulation of the Sox9 gene, resulting in an overgrowth phenotype. We now report that expression of the Dnmt2 RNA methyltransferase is required for the establishment and hereditary maintenance of both paramutations. Our data show that the Kit paramutant phenotype was not transmitted to the progeny of Dnmt2(-/-) mice and that the Sox9 paramutation was also not established in Dnmt2(-/-) embryos. Similarly, RNA from Dnmt2-negative Kit heterozygotes did not induce the paramutant phenotype when microinjected into Dnmt2-deficient fertilized eggs and microinjection of the miR-124 microRNA failed to induce the characteristic giant phenotype. In agreement with an RNA-mediated mechanism of inheritance, no change was observed in the DNA methylation profiles of the Kit locus between the wild-type and paramutant mice. RNA bisulfite sequencing confirmed Dnmt2-dependent tRNA methylation in mouse sperm and also indicated Dnmt2-dependent cytosine methylation in Kit RNA in paramutant embryos. Together, these findings uncover a novel function of Dnmt2 in RNA-mediated epigenetic heredity.
url http://europepmc.org/articles/PMC3662642?pdf=render
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