Title of article
A biaryl peptide crosslink in a MetJ peptide model confers cooperative, nonspecific binding to DNA that ablates both repressor binding and In vitro transcription Original Research Article
Author/Authors
Joshua C. Yoburn، نويسنده , , Sipra Deb، نويسنده , , Iain W. Manfield، نويسنده , , Lars Liljas and Peter G. Stockley، نويسنده , , David L.Van Vranken، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2003
Pages
6
From page
811
To page
816
Abstract
The MetJ repressor is the archetypal example of the β-ribbon-helix-helix DNA binding motif. A model of the MetJ β-ribbon (residues 22–28) was prepared by forming a dityrosine crosslinked dimer from the heptapeptide KKYTVSI. Using SPR, the peptide dimer 2 was shown to bind to dsDNA under physiologically relevant conditions, whereas the monomeric peptide did not. The peptide dimer appeared to inhibit binding of the MetJ repressor to natural met operators. Based on the stoichiometry of binding, the binding of peptide dimer 2 seems both highly co-operative and to lack sequence specificity. Peptide binding also appears to prevent transcription in vitro.
Journal title
Bioorganic and Medicinal Chemistry
Serial Year
2003
Journal title
Bioorganic and Medicinal Chemistry
Record number
1302572
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