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Literature DB >> 15049842

Thioether side chain cyclization for helical peptide formation: inhibitors of estrogen receptor-coactivator interactions.

A K Galande¹, K S Bramlett, T P Burris, J L Wittliff, A F Spatola.

Abstract

Cystine, lanthionine, and cystathionine containing cyclic peptides incorporating the signature nuclear receptor (NR) box (LXXLL) motif have been synthesized and the abilities of these peptides to inhibit estrogen receptor (ER)-coactivator interactions have been determined. We found that helicity of these peptides directly correlated with their bioactivity. Cystathionine proved to be a redox-stable, isosteric replacement for the cystine disulfide. Cystathionine containing peptide 3 showed higher helical character and a lower inhibition constant (Ki, 7 nm) when compared with its cystine counterpart.

Entities: Chemical Gene

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Year: 2004 PMID： 15049842 DOI： 10.1111/j.1399-3011.2004.00152.x

Source DB: PubMed Journal: J Pept Res ISSN： 1397-002X

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Cited

12 in total

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Review 3. Progress in lanthanides as luminescent probes.

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4. Bridged Analogues for p53-Dependent Cancer Therapy Obtained by S-Alkylation.

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Journal: Int J Pept Res Ther Date: 2015-08-19 Impact factor: 1.931

Review 5. Minireview: Not picking pockets: nuclear receptor alternate-site modulators (NRAMs).

Authors: Terry W Moore; Christopher G Mayne; John A Katzenellenbogen
Journal: Mol Endocrinol Date: 2009-11-20

6. Bicyclo[2.2.2]octanes: close structural mimics of the nuclear receptor-binding motif of steroid receptor coactivators.

Authors: Hai-Bing Zhou; Margaret L Collins; Jillian R Gunther; John S Comninos; John A Katzenellenbogen
Journal: Bioorg Med Chem Lett Date: 2007-05-23 Impact factor: 2.823

Thioether side chain cyclization for helical peptide formation: inhibitors of estrogen receptor-coactivator interactions.

Review 1. Inhibition of α-helix-mediated protein-protein interactions using designed molecules.

Review 2. Steroid receptor coactivators 1, 2, and 3: critical regulators of nuclear receptor activity and steroid receptor modulator (SRM)-based cancer therapy.

Review 3. Progress in lanthanides as luminescent probes.

4. Bridged Analogues for p53-Dependent Cancer Therapy Obtained by S-Alkylation.

Review 5. Minireview: Not picking pockets: nuclear receptor alternate-site modulators (NRAMs).

6. Bicyclo[2.2.2]octanes: close structural mimics of the nuclear receptor-binding motif of steroid receptor coactivators.

7. Synthesis and biological evaluation of guanylhydrazone coactivator binding inhibitors for the estrogen receptor.

Review 8. Inhibitors for the Vitamin D Receptor-Coregulator Interaction.

Review 9. Structure-Based Design of Inhibitors of Protein-Protein Interactions: Mimicking Peptide Binding Epitopes.

Review 10. Strategies for the development of conotoxins as new therapeutic leads.