Distinctive Klf4 mutants determine preference for DNA methylation status

We examined the role of Glu446 by mutagenesis. Substituting Glu446 with aspartate (E446D) resulted in preference for unmodified cytosine, due to decreased affinity for 5mC. In contrast, substituting Glu446 with proline (E446P) increased affinity for 5mC by two orders of magnitude. Structural analysis revealed hydrophobic interaction between the proline's aliphatic cyclic structure and the 5-methyl group of the pyrimidine (5mC or T). As in wild-type Klf4 (E446), the proline at position 446 does not interact directly with either the 5mC N4 nitrogen or the thymine O4 oxygen. In contrast, the unmethylated cytosine's exocyclic N4 amino group (NH2) and its ring carbon C5 atom hydrogen bond directly with the aspartate carboxylate of the E446D variant. Both of these interactions would provide a preference for cytosine over thymine, and the latter one could explain the E446D preference for unmethylated cytosine. Finally, we evaluated the ability of these Klf4 mutants to regulate transcription of methylated and unmethylated promoters in a luciferase reporter assay.

http://nar.oxfordjournals.org/cgi/content/short/44/21/10177?rss=1

Source: Nucleic Acids Research - December 1, 2016 Category: Research Authors: Hashimoto, H., Wang, D., Steves, A. N., Jin, P., Blumenthal, R. M., Zhang, X., Cheng, X. Tags: Gene regulation, Chromatin and Epigenetics Source Type: research

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