Please use this identifier to cite or link to this item: https://hdl.handle.net/2440/131378
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Type: Journal article
Title: Approaches to introduce helical structure in cysteine-containing peptides with a bimane group
Author: Horsfall, A.J.
McDougal, D.P.
Scanlon, D.B.
Bruning, J.B.
Abell, A.D.
Citation: ChemBioChem: a European journal of chemical biology, 2021; 22(17):2711-2720
Publisher: Wiley
Issue Date: 2021
ISSN: 1439-4227
1439-7633
Statement of
Responsibility: 
Aimee J. Horsfall, Daniel P. McDougal, Denis B. Scanlon, John B. Bruning, Andrew D. Abell
Abstract: An i-i+4 or i-i+3 bimane-containing linker was introduced into a peptide known to target Estrogen Receptor alpha (ERα) in order to stabilise an α-helical geometry. These macrocycles were studied by CD and NMR to reveal the i-i+4 constrained peptide adopts a 310-helical structure in solution, and an α-helical conformation on interaction with the ERα coactivator recruitment surface in silico. An acyclic bimane-modified peptide is also helical, when it includes a tryptophan or tyrosine residue; but is significantly less helical with a phenylalanine or alanine residue, which indicates such a bimane modification influences peptide structure in a sequence dependent manner. The fluorescence intensity of the bimane appears influenced by peptide conformation, where helical peptides displayed a fluorescence increase when TFE was added to phosphate buffer, compared to a decrease for less helical peptides. This study presents the bimane as a useful modification to influence peptide structure as an acyclic peptide modification, or as a side-chain constraint to give a macrocycle.
Keywords: Bimane
Helical structures
Peptidomimetics
fluorescence
peptides
Description: First published: 09 June 2021
Rights: © 2021 Wiley-VCH GmbH
DOI: 10.1002/cbic.202100241
Grant ID: http://purl.org/au-research/grants/arc/CE140100003
Published version: http://dx.doi.org/10.1002/cbic.202100241
Appears in Collections:Aurora harvest 8
Pharmacology publications

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