Literature DB >> 9461465

Multiple domains are involved in the targeting of the mouse DNA methyltransferase to the DNA replication foci.

Y Liu1, E J Oakeley, L Sun, J P Jost.   

Abstract

It has been shown that, during the S-phase of the cell cycle, the mouse DNA methyltransferase (DNA MTase) is targeted to sites of DNA replication by an amino acid sequence (aa 207-455) lying in the N-terminal domain of the enzyme [Leonhardt, H., Page, A. W., Weier, H. U. and Bestor, T. H. (1992) Cell , 71, 865-873]. In this paper it is shown, by using enhanced green fluorescent protein (EGFP) fusions, that other peptide sequences of DNA MTase are also involved in this targeting. The work focuses on a sequence, downstream of the reported targeting sequence (TS), which is homologous to the Polybromo-1 protein. This motif (designated as PBHD) is separated from the reported targeting sequence by a zinc-binding motif [Bestor , T. H. (1992) EMBO J , 11, 2611-2617]. Primed in situ extension using centromeric-specific primers was used to show that both the host DNA MTase and EGFP fusion proteins containing the targeting sequences were localized to centromeric, but not telomeric, regions during late S-phase and mitosis. Also found was that, in approximately 10% of the S-phase cells, the EGFP fusions did not co-localize with the centromeric regions. Mutants containing either, or both, of these targeting sequences could act as dominant negative mutants against the host DNA MTase. EGFP fusion proteins, containing the reported TS (aa 207-455), were targeted to centromeric regions throughout the mitotic stage which lead to the discovery of a similar behavior of the endogenous DNA MTase although the host MTase showed much less intense staining than in S-phase cells. The biological role of the centromeric localization of DNA MTase during mitosis is currently unknown.

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Year:  1998        PMID: 9461465      PMCID: PMC147368          DOI: 10.1093/nar/26.4.1038

Source DB:  PubMed          Journal:  Nucleic Acids Res        ISSN: 0305-1048            Impact factor:   16.971


  29 in total

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2.  Peptide mapping of the murine DNA methyltransferase reveals a major phosphorylation site and the start of translation.

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3.  High-efficiency transformation of mammalian cells by plasmid DNA.

Authors:  C Chen; H Okayama
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4.  Intracellular distribution of DNA methyltransferase during the cell cycle.

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5.  Localization of DNA methyltransferase in the chromatin of Friend erythroleukemia cells.

Authors:  F Creusot; J K Christman
Journal:  Nucleic Acids Res       Date:  1981-10-24       Impact factor: 16.971

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Journal:  Anal Biochem       Date:  1985-11-01       Impact factor: 3.365

7.  Replication of chromatin in mouse mammary epithelial cells grown in vitro.

Authors:  K Church
Journal:  Genetics       Date:  1965-10       Impact factor: 4.562

8.  Is the centromeric heterochromatin of Mus musculus late replicating?

Authors:  O J Miller
Journal:  Chromosoma       Date:  1976-04-21       Impact factor: 4.316

9.  Characteristics of enzymatic DNA methylation in cultured cells of human and hamster origin, and the effect of DNA replication inhibition.

Authors:  D M Woodcock; J K Adams; I A Cooper
Journal:  Biochim Biophys Acta       Date:  1982-01-26

10.  Regulation of mouse satellite DNA replication time.

Authors:  S Selig; M Ariel; R Goitein; M Marcus; H Cedar
Journal:  EMBO J       Date:  1988-02       Impact factor: 11.598

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  37 in total

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7.  Replication-independent chromatin loading of Dnmt1 during G2 and M phases.

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8.  Maintenance DNA methyltransferase (Met1) and silencing of CpG-methylated foreign DNA in Volvox carteri.

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9.  Direct interaction between DNMT1 and G9a coordinates DNA and histone methylation during replication.

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10.  DNA-methyltransferase 1 mRNA is selectively overexpressed in telencephalic GABAergic interneurons of schizophrenia brains.

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