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Azepinone-Containing Tetrapeptide Analogues of Melanotropin Lead to Selective hMC4R Agonists and hMC5R Antagonist.

Journal Contribution - Journal Article

Subtitle:IF 3.355

To address the need for highly potent, metabolically stable, and selective agonists, antagonists, and inverse agonists at the melanocortin receptor subtypes, conformationally constrained indolo- and benzazepinone residues were inserted into the α-MSH pharmacophore, His(6)-Phe(7)-Arg(8)-Trp(9)-domain. Replacement of His(6) by an aminoindoloazepinone (Aia) or aminobenzazepinone (Aba) moiety led to hMC4R and hMC5R selective agonist and antagonist ligands, respectively (tetrapeptides 1 to 3 and 4, respectively). In peptides 1 to 3 and depending on the para-substituent of the d-Phe residue in position 2, the activity goes from allosteric partial agonism (1, R = H) to allosteric full agonism (2, R = F) and finally allosteric partial agonism (3, R = Br).

Journal: ACS Medicinal Chemistry Letters
ISSN: 1948-5875
Issue: 2
Volume: 6
Pages: 192-197
Publication year:2015
Keywords:Organic & medicinal chemistry
  • PubMed Central Id: PMC4329577
  • WoS Id: 000349652000016
  • Scopus Id: 84922843034
CSS-citation score:1
Accessibility:Closed