Disruption of DNA-methylation-dependent long gene repression in Rett syndrome

Harrison W. Gabel; Benyam Kinde; Hume Stroud; Caitlin S. Gilbert; David A. Harmin; Nathaniel R. Kastan; Martin Hemberg; Daniel H. Ebert; Michael E. Greenberg

doi:10.1038/nature14319

Disruption of DNA-methylation-dependent long gene repression in Rett syndrome

Harrison W. Gabel, Benyam Kinde, Hume Stroud, Caitlin S. Gilbert, David A. Harmin, Nathaniel R. Kastan, Martin Hemberg, Daniel H. Ebert, Michael E. Greenberg

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373 Scopus citations

Abstract

Disruption of the MECP2 gene leads to Rett syndrome (RTT), a severe neurological disorder with features of autism. MECP2 encodes a methyl-DNA-binding protein that has been proposed to function as a transcriptional repressor, but despite numerous mouse studies examining neuronal gene expression in Mecp2 mutants, no clear model has emerged for how MeCP2 protein regulates transcription. Here we identify a genome-wide length-dependent increase in gene expression in MeCP2 mutant mouse models and human RTT brains. We present evidence that MeCP2 represses gene expression by binding to methylated CA sites within long genes, and that in neurons lacking MeCP2, decreasing the expression of long genes attenuates RTT-associated cellular deficits. In addition, we find that long genes as a population are enriched for neuronal functions and selectively expressed in the brain. These findings suggest that mutations in MeCP2 may cause neurological dysfunction by specifically disrupting long gene expression in the brain.

Original language	English
Pages (from-to)	89-93
Number of pages	5
Journal	Nature
Volume	522
Issue number	7554
DOIs	https://doi.org/10.1038/nature14319
State	Published - Jun 4 2015

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title = "Disruption of DNA-methylation-dependent long gene repression in Rett syndrome",

abstract = "Disruption of the MECP2 gene leads to Rett syndrome (RTT), a severe neurological disorder with features of autism. MECP2 encodes a methyl-DNA-binding protein that has been proposed to function as a transcriptional repressor, but despite numerous mouse studies examining neuronal gene expression in Mecp2 mutants, no clear model has emerged for how MeCP2 protein regulates transcription. Here we identify a genome-wide length-dependent increase in gene expression in MeCP2 mutant mouse models and human RTT brains. We present evidence that MeCP2 represses gene expression by binding to methylated CA sites within long genes, and that in neurons lacking MeCP2, decreasing the expression of long genes attenuates RTT-associated cellular deficits. In addition, we find that long genes as a population are enriched for neuronal functions and selectively expressed in the brain. These findings suggest that mutations in MeCP2 may cause neurological dysfunction by specifically disrupting long gene expression in the brain.",

author = "Gabel, {Harrison W.} and Benyam Kinde and Hume Stroud and Gilbert, {Caitlin S.} and Harmin, {David A.} and Kastan, {Nathaniel R.} and Martin Hemberg and Ebert, {Daniel H.} and Greenberg, {Michael E.}",

note = "Funding Information: Acknowledgements We thank E. Griffith and members of the Greenberg laboratory, A. Bird, G. Mandel and members of their laboratories, and M. Coenraads for discussions, M. Goodell for providing the Dnmt3a mice, N. Sharma and F. DiBiase for experimental support, and M. Mistry of the HSPH Bioinformatics Core, Harvard School of Public Health for assistance with gene expression analysis. This work was supported by grants from the Rett Syndrome Research Trust and the National Institutes of Health (NIH) (1RO1NS048276) to M.E.G., fellowships from the Damon Runyon Cancer Research Foundation (DRG-2048-10) and the William Randolf Hearst fund to H.W.G., as well as NIH grant T32GM007753, and the HHMI Gilliam fellowship to B.K., H.S. is a HHMI Fellow of the Damon Runyon Cancer Research Foundation (DRG-2194-14). Publisher Copyright: {\textcopyright} 2015 Macmillan Publishers Limited. All rights reserved.",

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doi = "10.1038/nature14319",

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AU - Gabel, Harrison W.

AU - Kinde, Benyam

AU - Stroud, Hume

AU - Gilbert, Caitlin S.

AU - Harmin, David A.

AU - Kastan, Nathaniel R.

AU - Hemberg, Martin

AU - Ebert, Daniel H.

AU - Greenberg, Michael E.

N1 - Funding Information: Acknowledgements We thank E. Griffith and members of the Greenberg laboratory, A. Bird, G. Mandel and members of their laboratories, and M. Coenraads for discussions, M. Goodell for providing the Dnmt3a mice, N. Sharma and F. DiBiase for experimental support, and M. Mistry of the HSPH Bioinformatics Core, Harvard School of Public Health for assistance with gene expression analysis. This work was supported by grants from the Rett Syndrome Research Trust and the National Institutes of Health (NIH) (1RO1NS048276) to M.E.G., fellowships from the Damon Runyon Cancer Research Foundation (DRG-2048-10) and the William Randolf Hearst fund to H.W.G., as well as NIH grant T32GM007753, and the HHMI Gilliam fellowship to B.K., H.S. is a HHMI Fellow of the Damon Runyon Cancer Research Foundation (DRG-2194-14). Publisher Copyright: © 2015 Macmillan Publishers Limited. All rights reserved.

PY - 2015/6/4

Y1 - 2015/6/4

N2 - Disruption of the MECP2 gene leads to Rett syndrome (RTT), a severe neurological disorder with features of autism. MECP2 encodes a methyl-DNA-binding protein that has been proposed to function as a transcriptional repressor, but despite numerous mouse studies examining neuronal gene expression in Mecp2 mutants, no clear model has emerged for how MeCP2 protein regulates transcription. Here we identify a genome-wide length-dependent increase in gene expression in MeCP2 mutant mouse models and human RTT brains. We present evidence that MeCP2 represses gene expression by binding to methylated CA sites within long genes, and that in neurons lacking MeCP2, decreasing the expression of long genes attenuates RTT-associated cellular deficits. In addition, we find that long genes as a population are enriched for neuronal functions and selectively expressed in the brain. These findings suggest that mutations in MeCP2 may cause neurological dysfunction by specifically disrupting long gene expression in the brain.

AB - Disruption of the MECP2 gene leads to Rett syndrome (RTT), a severe neurological disorder with features of autism. MECP2 encodes a methyl-DNA-binding protein that has been proposed to function as a transcriptional repressor, but despite numerous mouse studies examining neuronal gene expression in Mecp2 mutants, no clear model has emerged for how MeCP2 protein regulates transcription. Here we identify a genome-wide length-dependent increase in gene expression in MeCP2 mutant mouse models and human RTT brains. We present evidence that MeCP2 represses gene expression by binding to methylated CA sites within long genes, and that in neurons lacking MeCP2, decreasing the expression of long genes attenuates RTT-associated cellular deficits. In addition, we find that long genes as a population are enriched for neuronal functions and selectively expressed in the brain. These findings suggest that mutations in MeCP2 may cause neurological dysfunction by specifically disrupting long gene expression in the brain.

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Disruption of DNA-methylation-dependent long gene repression in Rett syndrome

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