Structure-Based Design of Melanocortin 4 Receptor Ligands Based on the SHU-9119-hMC4R Cocrystal Structure

Martin, Charlotte; Giménez, Luis E.; Williams, Savannah Y.; Yu, Jun; Wu, Yiran; Hollanders, Karlijn; Poorten, Olivier Van der; González, Sergio; holsbeeck, Kevin Van; Previti, Santo; Lamouroux, Arthur; Zhao, Suwen; Tourwé, Dirk; Stevens, Raymond C.; Cone, Roger D.; Ballet, Steven

doi:10.1021/acs.jmedchem.0c01620

Cited by 14 publications

(24 citation statements)

References 32 publications

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“…In the case of the MC4 receptor, the reference compound SHU9119 exhibits subnanomolar affinity with IC 50 = 0.15 nM. This is consistent with a recent report by Martin et al who found for this compound Ki = 0.029 nM [ 30 ]. All our hybrid peptidomimetics display potent binding to MC4R.…”

Section: Resultssupporting

confidence: 89%

Bifunctional Opioid/Melanocortin Peptidomimetics for Use in Neuropathic Pain: Variation in the Type and Length of the Linker Connecting the Two Pharmacophores

Witkowska

Godlewska

Osiejuk

et al. 2022

IJMS

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Based on the mechanism of neuropathic pain induction, a new type of bifunctional hybrid peptidomimetics was obtained for potential use in this type of pain. Hybrids consist of two types of pharmacophores that are connected by different types of linkers. The first pharmacophore is an opioid agonist, and the second pharmacophore is an antagonist of the pronociceptive system, i.e., an antagonist of the melanocortin-4 receptor. The results of tests in acute and neuropathic pain models of the obtained compounds have shown that the type of linker used to connect pharmacophores had an effect on antinociceptive activity. Peptidomimetics containing longer flexible linkers were very effective at low doses in the neuropathic pain model. To elucidate the effect of linker lengths, two hybrids showing very high activity and two hybrids with lower activity were further tested for affinity for opioid (mu, delta) and melanocortin-4 receptors. Their complexes with the target receptors were also studied by molecular modelling. Our results do not show a simple relationship between linker length and affinity for particular receptor types but suggest that activity in neuropathic pain is related to a proper balance of receptor affinity rather than maximum binding to any or all of the target receptors.

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Section: Resultssupporting

confidence: 89%

Bifunctional Opioid/Melanocortin Peptidomimetics for Use in Neuropathic Pain: Variation in the Type and Length of the Linker Connecting the Two Pharmacophores

Witkowska

Godlewska

Osiejuk

et al. 2022

IJMS

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“…Interestingly, SHU-9119 remained a full agonist at the hMC1R and hMC5R and had weak partial agonist activity at the hMC3R 28 . As this was reported in 1995, and other publications also documented the association between DNal(2’) 7 and MC3R/MC4R antagonism or weak partial agonism 31 , we sought to determine if the DNal(2’) 7 residue might be a general marker of MC3R/MC4R antagonism. If so, we might then have a diagnostic tool for peptide mischaracterization over history since this DNal(2’) 7 change was frequently included in many series of melanocortin peptides designed in a variety of labs and then characterized pharmacologically at the University of Arizona.…”

Section: Resultsmentioning

confidence: 88%

Demonstration of a common DPhe⁷ to DNal(2’)⁷ peptide ligand antagonist switch for the melanocortin-3 and melanocortin-4 receptors identifies systematic mischaracterization of the pharmacological properties of melanocortin peptides

Giménez

Noblin

Williams

et al. 2022

Preprint

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Melanocortin peptides containing a D-naphthylalanine residue in position 7 (DNal(2')7), reported as melanocortin-3 receptor (MC3R) subtype-specific agonists in two separate publications, were found to lack significant MC3R agonist activity. The cell lines used at the University of Arizona for pharmacological characterization of these peptides, consisting of HEK293 cells stably transfected with human melanocortin receptor subtypes MC1R, MC3R, MC4R, or MC5R, were then obtained and characterized by quantitative PCR. While the MC1R cell line correctly expressed only the hMCR1, the three other cell lines were mischaracterized with regard to receptor subtype expression. Demonstration that a D-naphthylalanine residue in position 7, irrespective of the melanocortin peptide template, results primarily in antagonism of the MC3R and MC4R, then allowed us to search the published literature for additional errors. The erroneously characterized DNal(2')7-containing peptides date back to 2003; thus, our analysis suggests that systematic mischaracterization of the pharmacological properties of melanocortin peptides occurred.

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“…Given the prevalence of GPCR crystal structures over other MP classes, SBDD for GPCRs is the most advanced, with three small-molecule candidates from Sosei Heptares currently in clinical trials [36]. SBDD studies from the past 2 years (Table 2) demonstrate that solved crystal structures of GPCRs with ligands are enabling the design of more selective drugs with novel chemical structures [37][38][39]. When multiple active-state structures are available, as in the case of the β2-adrenergic receptor (β2AR), virtual screening can enable the design of sought-after agonists [40,41].…”

Section: Structure-based Drug Designmentioning

confidence: 99%

Membrane protein production and formulation for drug discovery

Gulezian

Crivello

Bednenko

et al. 2021

Trends in Pharmacological Sciences

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Structure-Based Design of Melanocortin 4 Receptor Ligands Based on the SHU-9119-hMC4R Cocrystal Structure

Cited by 14 publications

References 32 publications

Bifunctional Opioid/Melanocortin Peptidomimetics for Use in Neuropathic Pain: Variation in the Type and Length of the Linker Connecting the Two Pharmacophores

Bifunctional Opioid/Melanocortin Peptidomimetics for Use in Neuropathic Pain: Variation in the Type and Length of the Linker Connecting the Two Pharmacophores

Demonstration of a common DPhe⁷ to DNal(2’)⁷ peptide ligand antagonist switch for the melanocortin-3 and melanocortin-4 receptors identifies systematic mischaracterization of the pharmacological properties of melanocortin peptides

Membrane protein production and formulation for drug discovery

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Structure-Based Design of Melanocortin 4 Receptor Ligands Based on the SHU-9119-hMC4R Cocrystal Structure

Cited by 14 publications

References 32 publications

Bifunctional Opioid/Melanocortin Peptidomimetics for Use in Neuropathic Pain: Variation in the Type and Length of the Linker Connecting the Two Pharmacophores

Bifunctional Opioid/Melanocortin Peptidomimetics for Use in Neuropathic Pain: Variation in the Type and Length of the Linker Connecting the Two Pharmacophores

Demonstration of a common DPhe7 to DNal(2’)7 peptide ligand antagonist switch for the melanocortin-3 and melanocortin-4 receptors identifies systematic mischaracterization of the pharmacological properties of melanocortin peptides

Membrane protein production and formulation for drug discovery

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Demonstration of a common DPhe⁷ to DNal(2’)⁷ peptide ligand antagonist switch for the melanocortin-3 and melanocortin-4 receptors identifies systematic mischaracterization of the pharmacological properties of melanocortin peptides