2000
DOI: 10.1021/jm000211e
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d-Amino Acid Scan of γ-Melanocyte-Stimulating Hormone:  Importance of Trp8 on Human MC3 Receptor Selectivity

Abstract: In our search for potent and receptor-selective agonists and antagonists, we report here the results of D-amino acid substitution at each position of the short peptide gamma-melanocyte-stimulating hormone (gamma-MSH). The native gamma-MSH shows weak binding at all three receptors (i.e., the human MC3, MC4, and MC5) and a selectivity of 1-2 orders of magnitude at the MC3R over the MC4R and MC5R. Sequential replacement of each residue in the gamma-MSH sequence with the corresponding D-isomer results in analogues… Show more

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Cited by 114 publications
(156 citation statements)
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“…We have done so by using a pharmacological, genetic and molecular approach utilising the selective MC3R ligand [D-TRP 8 ]-γ-MSH, [24,25], MC3R deficient mice [28,31] and the recessive yellow e/e (bearing a nonfunctional MC1R) mouse [14]. This study has focused on the MC1 and 3R given the wealth of data highlighting that both these receptors are involved in modulating the host inflammatory response [10] other MCR were not evaluated in this study due to the fact that they haven't been implicated in modulating peripheral inflammation.…”
Section: Discussionmentioning
confidence: 99%
See 1 more Smart Citation
“…We have done so by using a pharmacological, genetic and molecular approach utilising the selective MC3R ligand [D-TRP 8 ]-γ-MSH, [24,25], MC3R deficient mice [28,31] and the recessive yellow e/e (bearing a nonfunctional MC1R) mouse [14]. This study has focused on the MC1 and 3R given the wealth of data highlighting that both these receptors are involved in modulating the host inflammatory response [10] other MCR were not evaluated in this study due to the fact that they haven't been implicated in modulating peripheral inflammation.…”
Section: Discussionmentioning
confidence: 99%
“…Following electrophorysis in a 10% polyacrylamide gel, membranes were blocked overnight in blocking solution containing 5% non-fat milk solution in Tris buffer saline containing 0.1% Tween-20 followed by anti-MC3R (1:2000) [22] synthesised by Dr Paolo Grieco as previously described [24,25], peptides were stored at -20°C prior to use, and dissolved in sterile PBS (pH 7.4).…”
Section: Mcr Protein Expressionmentioning
confidence: 99%
“…9 A, C,D). D-Trp8-␥-MSH was used as a selective agonist of MC3R given its 40-to 200-fold selectivity over MC4R and MC5R (Grieco et al, 2000;Cowley et al, 2001). In all cells tested, D-Trp8-␥-MSH (10 nM) (1 min) also showed a consistent inhibition of GFP-VMH neurons (Fig.…”
Section: Effects Of Mc4r and Mc3r Selective Agonists On Glutamatergicmentioning
confidence: 99%
“…[e.g. 41,43]. Once the structure activity relationships (SAR) of the peptide ligand have been elucidated, the conformation-activity relationships have to be examined.…”
Section: General Considerations For the Design Of Hmc3r Selective Agomentioning
confidence: 99%
“…Biological screening demonstrated that γ-MSH was selective for the hMC3R by up to 100 fold, compared to α-MSH [49]. Grieco et al used a D-amino acid scan of the γ-MSH sequence to obtain the first highly selective agonist for the hMC3R (H-Tyr-Val-Met-Gly-His-Phe-Arg-D-Trp-Asp-Arg-PheGly-OH; EC 50 = 0.33 nM; hMC4R/hMC3R = 300, hMC5R/hMC3R = 250) [43]. Furthermore, replacement of the oxidizable Met 3 residue with Nle increased the stability of the peptide [52], which is being widely used as a ligand for the hMC3R in a variety of ongoing pharmacological studies and in animal model studies related to the hMC3R.…”
Section: Structure-activity Relationships Of Linear Msh-derived Peptidesmentioning
confidence: 99%