Issue 9, 2008

Proline-rich proteins—deriving a basis for residue-based selectivity in polyphenolic binding

Abstract

1H NMR titration experiments have been used to establish that minimal proline-based models show enhanced binding selectivity towards phenol in CDCl3, relative to other similarly protected amino acid residues. Cooperative binding effects appear to play a role, with sarcosine models affording binding constants to phenol intermediate to those obtained from proline models and other amino acid models. The mechanism for binding, based on DFT calculations and the application of Hunter's molecular recognition toolbox model, cannot be solely attributed to hydrogen bond strength, and appears to be mediated through C–H-π bonds and the rotational freedom of the amide substrate.

Graphical abstract: Proline-rich proteins—deriving a basis for residue-based selectivity in polyphenolic binding

Supplementary files

Article information

Article type
Paper
Submitted
09 Jan 2008
Accepted
22 Feb 2008
First published
19 Mar 2008

Org. Biomol. Chem., 2008,6, 1594-1600

Proline-rich proteins—deriving a basis for residue-based selectivity in polyphenolic binding

A. K. Croft and M. K. Foley, Org. Biomol. Chem., 2008, 6, 1594 DOI: 10.1039/B800365C

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