Multiple Modes of Interaction between the Methylated DNA Binding Protein MeCP2 and Chromatin

Nikitina, Tatiana; Xi, Sichuan; Ghosh, Rajarshi P.; Horowitz-Scherer, Rachel A.; Hansen, Jeffrey C.; Woodcock, Christopher L.

doi:10.1128/mcb.01593-06

Cited by 158 publications

(195 citation statements)

References 65 publications

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“…multiple chromatin interaction regions in addition to the MBD motif (21,22). In conclusion, the three MBD motifs in AtMBD7 were found to increase the protein binding affinity for chromatin and to determine its subnuclear localization and could potentially induce chromatin compaction of methylated CpG chromosomal regions.…”

Section: Resultsmentioning

confidence: 78%

The Three Methyl-CpG-binding Domains of AtMBD7 Control Its Subnuclear Localization and Mobility

Zemach

Gaspan

Grafi

2008

Journal of Biological Chemistry

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Three methyl-CpG-binding domain (MBD) proteins in Arabidopsis, AtMBD5, AtMBD6, and AtMBD7, are functional in binding methylated CpG dinucleotides in vitro and localize to the highly CpG-methylated chromocenters in vivo. These proteins differ, however, in their subnuclear localization pattern; AtMBD5 and AtMBD6, each containing a single MBD motif, show preference for two perinucleolar chromocenters, whereas AtMBD7, a naturally occurring poly-MBD protein containing three MBD motifs, localizes to all chromocenters. Here we studied the significance of multiple MBD motifs for subnuclear localization and mobility in living cells. We found that the number of MBD motifs determines the subnuclear localization of the MBD protein. Furthermore, live kinetic experiments showed that AtMBD7-green fluorescent protein (GFP) has lower mobility than AtMBD5-GFP and AtMBD6-GFP, which is conferred by cooperative activity of its three MBD motifs. Thus, the number of MBD motifs appears to affect not only binding affinity and mobility within the nucleus, but also the subnuclear localization of the protein. Our results suggest that poly-MBD proteins can directly affect chromatin structure by inducing intra-and interchromatin compaction via bridging over multiple methylated CpG sites.Cytosine methylation is a common epigenetic modification of most eukaryotic nuclear DNA. Intensive studies demonstrated the central role played by cytosine methylation in genome organization, gene expression, and growth and development. The way by which the methyl group is interpreted into a functional state has begun to be unraveled with the isolation and characterization of methylated DNA-binding proteins. This group of proteins includes an evolutionary conserved protein family, initially described in animals, termed methyl-CpGbinding domain (MBD) 2 proteins (1). Biochemical and molecular analyses suggest that mammalian MBDs induce the formation of a repressive chromatin structure at methylated CpG (mCpG) sites by the recruitment of various chromatin factors including histone deacetylases, histone methyltransferases, and ATPase-dependent nucleosome remodeling factors (2, 3). Thus far, of the 13 AtMBD proteins found in Arabidopsis, only AtMBD5, AtMBD6, and AtMBD7 were found to bind mCpG sites in vitro and to localize in vivo to the highly methylated chromocenters (ChCs) (reviewed in Refs. 4 and 5). This chromocenter localization is CpG methylation-dependent inasmuch as it was disrupted in the hypomethylated mutants ddm1 and met1 (6). Yet, these three AtMBDs display different localization patterns within Arabidopsis nuclei; AtMBD7 is predominantly localized at all ChCs, whereas AtMBD5 and AtMBD6 show preference for two perinucleolar ChCs adjacent to the ribosomal DNA clusters (6). A major structural feature distinguishing AtMBD7 from AtMBD5 and AtMBD6 is the presence of three MBD motifs within its protein sequence. Notably, naturally occurring poly-MBD proteins appear to be unique to plants as to date no such protein has been found in animals. Here we studied...

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Section: Resultsmentioning

confidence: 78%

The Three Methyl-CpG-binding Domains of AtMBD7 Control Its Subnuclear Localization and Mobility

Zemach

Gaspan

Grafi

2008

Journal of Biological Chemistry

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“…23,24 These studies implicate a role for the methyl CpG binding protein 2 (MeCP2), a key member of the methyl-DNA binding protein family of proteins. [25][26][27][28][29] While MeCP2 can bind to unmethylated DNA, 29 preferentially it binds methylated DNA at the 5=-CpG residues. 30 -31 MeCP2 is originally considered to be a transcriptional repressor in conjunction with Sin3A and histone deacetylase, but was found later to also have a significant role as a transcriptional activator, as well as in the regulation of chromatin architecture and RNA splicing.…”

Section: Dna Methylation Is a Key Mechanism For Repression Of Gene Exmentioning

confidence: 99%

Essential Role of MeCP2 in the Regulation of Myofibroblast Differentiation during Pulmonary Fibrosis

Gharaee−Kermani

et al. 2011

The American Journal of Pathology

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DNA methylation is a key mechanism for repression of gene expression, including that of ␣-smooth muscle actin (␣-SMA) gene expression in fibroblasts. However, the trans-acting factors that interact with the methylated ␣-SMA gene to regulate its expression have not been identified. Using gel shift and chromatin immunoprecipitation (ChIP) assays, methyl CpG binding protein 2 (MeCP2) was shown to bind to the ␣-SMA gene. Suppression of MeCP2 gene expression by siRNA or its deficiency in lung fibroblasts isolated from MeCP2 knockout mice caused significant reduction of ␣-SMA gene expression. In contrast, transient transfection of MeCP2 expression plasmid into fibroblasts enhanced ␣-SMA gene expression. Moreover, in vivo studies revealed that compared to their wild type littermates, MeCP2-deficient mice exhibited significantly decreased alveolar wall thickness, inflammatory cell infiltration, interstitial collagen deposition, and myofibroblast differentiation in response to endotracheal injection of bleomycin. Thus, MeCP2 is essential for myofibroblast differentiation and pulmonary fibrosis.

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“…More recent evidence suggests that Mecp2-null mice and Rett patients do not ectopically express genes that are regulated by promoter methylation (9,10). More diverse roles for MeCP2 have recently been shown in the direct compaction of chromatin (11,12) and the control of alternative splicing of pre-mRNA (13). The multifunctional nature of MeCP2 is reflected by its intrinsically disordered structure of multiple autonomous domains (14), including a methyl CpG-binding domain (MBD) (15) and a transcriptional repression domain (TRD) (8).…”

mentioning

confidence: 99%

Integrated epigenomic analyses of neuronal MeCP2 reveal a role for long-range interaction with active genes

Yasui¹,

Peddada²,

Bieda

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

339

303

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Mutations in MECP2 cause the autism-spectrum disorder Rett syndrome. MeCP2 is predicted to bind to methylated promoters and silence transcription. However, the first large-scale mapping of neuronal MeCP2-binding sites on 26.3 Mb of imprinted and nonimprinted loci revealed that 59% of MeCP2-binding sites are outside of genes and that only 6% are in CpG islands. Integrated genome-wide promoter analysis of MeCP2 binding, CpG methylation, and gene expression revealed that 63% of MeCP2-bound promoters are actively expressed and that only 6% are highly methylated. These results indicate that the primary function of MeCP2 is not the silencing of methylated promoters.chromatin ͉ DNA methylation ͉ epigenetics ͉ genomics ͉ Rett syndrome

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Multiple Modes of Interaction between the Methylated DNA Binding Protein MeCP2 and Chromatin

Cited by 158 publications

References 65 publications

The Three Methyl-CpG-binding Domains of AtMBD7 Control Its Subnuclear Localization and Mobility

The Three Methyl-CpG-binding Domains of AtMBD7 Control Its Subnuclear Localization and Mobility

Essential Role of MeCP2 in the Regulation of Myofibroblast Differentiation during Pulmonary Fibrosis

Integrated epigenomic analyses of neuronal MeCP2 reveal a role for long-range interaction with active genes

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