Structural junctions in DNA: the influence of flanking sequence on nuclease digestion specificities

doi:10.1093/nar/13.12.4445

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Nucleic Acids Research, 1985, Vol. 13, No. 12 4445-4467
© 1985

Articles

Structural junctions in DNA: the influence of flanking sequence on nuclease digestion specificities

Horace R. Drew and Andrew A. Travers

MRC Laboratory of Molecular Biology Hills Road, Cambridge CB2 2QH, UK

Received April 29, 1985. Revised May 24, 1985. Accepted May 24, 1985.

When a protein binds to DNA, the affinity of this protein forits primary site of interaction may be influenced by the natureof flanking sequences. This is thought to be a consequence oflocal cooperativity in the DNA molecule, where the conformationat one point along the helix can influence the conformationat another, and thereby modulate the free energy of protein-DNArecognition.

In order to learn more about this process, we have carried outexperiments of two sorts. First, we have constructed sequencesof the type (dA)₁₁ (dG)₈, where the conformational preferencesof the DNA molecule switch from one extreme to another overjust a single base pair, and subjected them to digestion byDNAase I and DNAase II. This is to learn whether the structurechanges abruptly at the Junction point, or more gradually withan influence extending into residues on either side. Secondly,we have subjected long plasmid DNA to digestion by restrictionenzymes Fnu DII, Hae III, Hha I and Msp I, to look for correlationsbetween cutting rate and the identity of nucleotides on eitherside of the restriction site.

The influence of flanking sequence on nuclease digestion specificitiesis clearly evident in both kinds of experiment, but the rulesgoverning this seem complex and not easily formulated. The bestthat can be done at present is to divide the problem into twoparts, "analogue" and "digital", representing sugar-phosphateand base components of recognition

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