Literature DB >> 28374217

Methylation-targeted specificity of the DNA binding proteins R.DpnI and MeCP2 studied by molecular dynamics simulations.

Siba Shanak1,2, Ozlem Ulucan1, Volkhard Helms3.   

Abstract

DNA methylation plays a major role in organismal development and the regulation of gene expression. Methylation of cytosine bases and the cellular roles of methylated cytosine in eukaryotes are well established, as well as methylation of adenine bases in bacterial genomes. Still lacking, however, is a general mechanistic understanding, in structural and thermodynamic terms, of how proteins recognize methylated DNA. Toward this aim, we present the results of molecular dynamics simulations, alchemical free energy perturbation, and MM-PBSA calculations to explain the specificity of the R.DpnI enzyme from Streptococcus pneumonia in binding to adenine-methylated DNA with both its catalytic and winged-helix domains. We found that adenine-methylated DNA binds more favorably to the catalytic subunit of R.DpnI (-4 kcal mol-1) and to the winged-helix domain (-1.6 kcal mol-1) than non-methylated DNA. In particular, N6-adenine methylation is found to enthalpically stabilize binding to R.DpnI. In contrast, C5-cytosine methylation entropically favors complexation by the MBD domain of the human MeCP2 protein with almost no contribution of the binding enthalpy.

Entities:  

Keywords:  Binding free energy; Conformational entropy; DNA methylation; Free energy perturbation; MM-PBSA; Restriction endonuclease; Sequence specificity; m5C; m6A

Mesh:

Substances:

Year:  2017        PMID: 28374217     DOI: 10.1007/s00894-017-3318-8

Source DB:  PubMed          Journal:  J Mol Model        ISSN: 0948-5023            Impact factor:   1.810


  32 in total

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6.  An atomic model of Zfp57 recognition of CpG methylation within a specific DNA sequence.

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7.  Hydration properties of natural and synthetic DNA sequences with methylated adenine or cytosine bases in the R.DpnI target and BDNF promoter studied by molecular dynamics simulations.

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9.  Recognition of methylated DNA through methyl-CpG binding domain proteins.

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10.  MeCP2, a key contributor to neurological disease, activates and represses transcription.

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