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Design of Sequence-Specific DNA Binding Molecules for DNA Methyltransferase Inhibition

[Image: see text] The CpG dyad, an important genomic feature in DNA methylation and transcriptional regulation, is an attractive target for small molecules. To assess the utility of minor groove binding oligomers for CpG recognition, we screened a small library of hairpin pyrrole-imidazole polyamide...

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Autores principales: Kang, JeenJoo S., Meier, Jordan L., Dervan, Peter B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2014
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3985849/
https://www.ncbi.nlm.nih.gov/pubmed/24502234
http://dx.doi.org/10.1021/ja500211z
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author Kang, JeenJoo S.
Meier, Jordan L.
Dervan, Peter B.
author_facet Kang, JeenJoo S.
Meier, Jordan L.
Dervan, Peter B.
author_sort Kang, JeenJoo S.
collection PubMed
description [Image: see text] The CpG dyad, an important genomic feature in DNA methylation and transcriptional regulation, is an attractive target for small molecules. To assess the utility of minor groove binding oligomers for CpG recognition, we screened a small library of hairpin pyrrole-imidazole polyamides targeting the sequence 5′-CGCG-3′ and assessed their sequence specificity using an unbiased next-generation sequencing assay. Our findings indicate that hairpin polyamide of sequence PyImβIm-γ-PyImβIm (1), previously identified as a high affinity 5′-CGCG-3′ binder, favors 5′-GCGC-3′ in an unanticipated reverse binding orientation. Replacement of one β alanine with Py to afford PyImPyIm-γ-PyImβIm (3) restores the preference for 5′-CGCG-3′ binding in a forward orientation. The minor groove binding hairpin 3 inhibits DNA methyltransferase activity in the major groove at its target site more effectively than 1, providing a molecular basis for design of sequence-specific antagonists of CpG methylation.
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spelling pubmed-39858492015-02-06 Design of Sequence-Specific DNA Binding Molecules for DNA Methyltransferase Inhibition Kang, JeenJoo S. Meier, Jordan L. Dervan, Peter B. J Am Chem Soc [Image: see text] The CpG dyad, an important genomic feature in DNA methylation and transcriptional regulation, is an attractive target for small molecules. To assess the utility of minor groove binding oligomers for CpG recognition, we screened a small library of hairpin pyrrole-imidazole polyamides targeting the sequence 5′-CGCG-3′ and assessed their sequence specificity using an unbiased next-generation sequencing assay. Our findings indicate that hairpin polyamide of sequence PyImβIm-γ-PyImβIm (1), previously identified as a high affinity 5′-CGCG-3′ binder, favors 5′-GCGC-3′ in an unanticipated reverse binding orientation. Replacement of one β alanine with Py to afford PyImPyIm-γ-PyImβIm (3) restores the preference for 5′-CGCG-3′ binding in a forward orientation. The minor groove binding hairpin 3 inhibits DNA methyltransferase activity in the major groove at its target site more effectively than 1, providing a molecular basis for design of sequence-specific antagonists of CpG methylation. American Chemical Society 2014-02-06 2014-03-05 /pmc/articles/PMC3985849/ /pubmed/24502234 http://dx.doi.org/10.1021/ja500211z Text en Copyright © 2014 American Chemical Society
spellingShingle Kang, JeenJoo S.
Meier, Jordan L.
Dervan, Peter B.
Design of Sequence-Specific DNA Binding Molecules for DNA Methyltransferase Inhibition
title Design of Sequence-Specific DNA Binding Molecules for DNA Methyltransferase Inhibition
title_full Design of Sequence-Specific DNA Binding Molecules for DNA Methyltransferase Inhibition
title_fullStr Design of Sequence-Specific DNA Binding Molecules for DNA Methyltransferase Inhibition
title_full_unstemmed Design of Sequence-Specific DNA Binding Molecules for DNA Methyltransferase Inhibition
title_short Design of Sequence-Specific DNA Binding Molecules for DNA Methyltransferase Inhibition
title_sort design of sequence-specific dna binding molecules for dna methyltransferase inhibition
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3985849/
https://www.ncbi.nlm.nih.gov/pubmed/24502234
http://dx.doi.org/10.1021/ja500211z
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