4.6 Article

Cooperative DNA Binding and Protein/DNA Fiber Formation Increases the Activity of the Dnmt3a DNA Methyltransferase

Journal

JOURNAL OF BIOLOGICAL CHEMISTRY
Volume 289, Issue 43, Pages 29602-29613

Publisher

AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC
DOI: 10.1074/jbc.M114.572032

Keywords

Cooperativity; DNA Enzyme; DNA Methylation; DNA Methyltransferase; Enzyme Kinetics; Enzyme Mechanism

Funding

  1. Deutsche Forschungsgemeinschaft [JE 252/10]
  2. Bundesministerium fur Bildung und Forschung [FKZ 01GS0805]

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Background: Dnmt3a has been reported to multimerize on DNA and methylate DNA processively, which is contradicting. Results: We show that multimerization of Dnmt3a on DNA increases its activity, but processive DNA methylation is not detectable. Conclusion: Dnmt3a forms enzyme/DNA fibers. Significance: Our results help to understand the mechanism of DNA methylation and the effects of Dnmt3a somatic cancer mutations. The Dnmt3a DNA methyltransferase has been shown to bind cooperatively to DNA and to form large multimeric protein/DNA fibers. However, it has also been reported to methylate DNA in a processive manner, a property that is incompatible with protein/DNA fiber formation. We show here that the DNA methylation rate of Dnmt3a increases more than linearly with increasing enzyme concentration on a long DNA substrate, but not on a short 30-mer oligonucleotide substrate. We also show that addition of a catalytically inactive Dnmt3a mutant, which carries an amino acid exchange in the catalytic center, increases the DNA methylation rate by wild type Dnmt3a on the long substrate but not on the short one. In agreement with this finding, preincubation experiments indicate that stable protein/DNA fibers are formed on the long, but not on the short substrate. In addition, methylation experiments with substrates containing one or two CpG sites did not provide evidence for a processive mechanism over a wide range of enzyme concentrations. These data clearly indicate that Dnmt3a binds to DNA in a cooperative reaction and that the formation of stable protein/DNA fibers increases the DNA methylation rate. Fiber formation occurs at low m concentrations of Dnmt3a, which are in the range of Dnmt3a concentrations in the nucleus of embryonic stem cells. Understanding the mechanism of Dnmt3a is of vital importance because Dnmt3a is a hotspot of somatic cancer mutations one of which has been implicated in changing Dnmt3a processivity.

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