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Preferred binding sites for the bifunctional intercalator TANDEM determined using DNA fragments that contain every symmetrical hexanucleotide sequence

Preferred binding sites for the bifunctional intercalator TANDEM determined using DNA fragments that contain every symmetrical hexanucleotide sequence
Preferred binding sites for the bifunctional intercalator TANDEM determined using DNA fragments that contain every symmetrical hexanucleotide sequence
We have prepared novel DNA footprinting substrates that contain all 64 symmetrical hexanucleotide sequences. These were contained in two restriction fragments that were cloned into the pUC19 polylinker site; each fragment was also obtained in both orientations. These fragments were used to assess the sequence binding preferences of the synthetic quinoxaline antibiotic TANDEM. We found that, although the ligand binds to most TpA steps, the affinity is affected by the flanking sequences. The best binding sites contain the tetranucleotide sequence ATAT, although YATATR is a better site than RATATY. TTAA always is a poor binding site, especially TTTAAA. The binding to GTAC is strongly dependent on the flanking bases, with good binding to GGTACC but none at all to CGTACG.
0003-2697
298-303
Hampshire, Andrew J.
68aac3b7-88b7-4417-8793-9c2a06b01abc
Fox, Keith R.
9da5debc-4e45-473e-ab8c-550d1104659f
Hampshire, Andrew J.
68aac3b7-88b7-4417-8793-9c2a06b01abc
Fox, Keith R.
9da5debc-4e45-473e-ab8c-550d1104659f

Hampshire, Andrew J. and Fox, Keith R. (2008) Preferred binding sites for the bifunctional intercalator TANDEM determined using DNA fragments that contain every symmetrical hexanucleotide sequence. Analytical Biochemistry, 374 (2), 298-303. (doi:10.1016/j.ab.2007.10.008).

Record type: Article

Abstract

We have prepared novel DNA footprinting substrates that contain all 64 symmetrical hexanucleotide sequences. These were contained in two restriction fragments that were cloned into the pUC19 polylinker site; each fragment was also obtained in both orientations. These fragments were used to assess the sequence binding preferences of the synthetic quinoxaline antibiotic TANDEM. We found that, although the ligand binds to most TpA steps, the affinity is affected by the flanking sequences. The best binding sites contain the tetranucleotide sequence ATAT, although YATATR is a better site than RATATY. TTAA always is a poor binding site, especially TTTAAA. The binding to GTAC is strongly dependent on the flanking bases, with good binding to GGTACC but none at all to CGTACG.

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Published date: 15 March 2008
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Identifiers

Local EPrints ID: 142567
URI: http://eprints.soton.ac.uk/id/eprint/142567
DOI: doi:10.1016/j.ab.2007.10.008
ISSN: 0003-2697
PURE UUID: 84b052b7-4772-470e-b241-21b551c5dbd6
ORCID for Keith R. Fox: ORCID iD orcid.org/0000-0002-2925-7315

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Date deposited: 01 Apr 2010 15:34
Last modified: 14 Mar 2024 02:33

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Contributors

Author: Andrew J. Hampshire
Author: Keith R. Fox ORCID iD

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