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(Received for publication, September 22, 1994; and in revised form, December 18, 1994) The restriction endonuclease EcoRI binds and cleaves
DNA containing GAATTC sequences with high specificity. According to the
crystal structure, most of the specific contacts of the enzyme to the
DNA are formed by the extended chain region and the first turn of
Volume 270,
Number 10,
Issue of March 10, 1995 pp. 5122-5129
©1995 by The American Society for Biochemistry and Molecular Biology, Inc.
4 Region of the
Restriction Endonuclease EcoRI Specifically Binds to the EcoRI Recognition Site
-helix
4 (amino acids 137-145). Here, we demonstrate
that a dodecapeptide (WDGMAAGNAIER), which is identical in the
underlined parts of its sequence to EcoRI amino acids
137-145, specifically binds to GAATTC sequences. The peptide
inhibits DNA cleavage by EcoRI but not by BamHI, BclI, EcoRV, HindIII, PacI, and XbaI. DNA cleavage by XbaI is slowed down at sites
that partially overlap with EcoRI sites. The peptide inhibits
cleavage of GAATTC sites by ApoI, which recognizes the
sequence RAATTY. It interferes with DNA methylation by the EcoRI methyltransferase but not by the BamHI
methyltransferase. It competes with EcoRI for DNA binding.
Based on these results, the DNA binding constant of the peptide to
GAATTC sequences was calculated to be 3 10
M
. DNA binding is not
temperature-dependent, suggesting that binding of the peptide is
entropy-driven. As the peptide does not show any nonspecific binding to
DNA, its DNA binding specificity is similar to that of EcoRI,
in spite of the fact that the affinity is much smaller. These results
suggest that contacts to the phosphate groups in EcoRI mainly
provide binding affinity, whereas the specificity of EcoRI is
based to a large extent on sequence-specific base contacts.
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