Dimeric argininamide-type neuropeptide Y receptor antagonists: Chiral discrimination between Y1 and Y4 receptors

Keller, Max; Kaske, Melanie; Holzammer, Tobias; Bernhardt, Günther; Buschauer, Armin

doi:10.1016/j.bmc.2013.08.065

Cited by 18 publications

(55 citation statements)

References 29 publications

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“…The adamantyl substitution completely mimicked the potency and maximum response of the carbaboranylated peptide (Figure A). As short peptide analogues of NPY were reported to be active at the related hY 4 R, we also investigated signalling at this receptor (Figure B). Although all of these peptides were able to activate hY 4 R, it was only at very high concentrations, which led to selectivity for hY 1 R over hY 4 R for all modified truncated analogues ranging from 4.4‐fold selectivity for Phe‐sNPY to 237‐fold selectivity for Lau‐sNPY.…”

Section: Resultsmentioning

confidence: 99%

“…[6] Substitution of the N e -amino group of the Lyss ide chain led to improved potencies in all cases relative to sNPY.T here is ac lear correlation between hydrophobicity and potencyf or the truncated analogues, and the phenyls ubstitution is the least active one and the lauroyl chain is the most active one, resembling NPY activity.T he adamantyl substitution completely mimicked the potencya nd maximum response of the carbaboranylated peptide (Figure 2A). As short peptide analogueso fN PY were reported to be active at the relatedh Y 4 R, [11] we also investigated signalling at this receptor ( Figure 2B). Althougha ll of these peptides were able to activate hY 4 R, it was only at very high concentrations, which led to selectivityf or hY 1 Ro ver hY 4 Rf or all modified truncated analogues ranging from 4.4-fold selectivity for Phe-sNPY to 237-fold selectivity for Lau-sNPY.…”

Section: G-protein Signallingmentioning

confidence: 99%

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Carbaboranylation of Truncated C‐Terminal Neuropeptide Y Analogue Leads to Full hY₁ Receptor Agonism

et al. 2018

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The human Y receptor is overexpressed in breast tumour cells and is, therefore, a valuable target for site-selective drug delivery. The well-established hY R-selective ligand [Phe7,Pro34]NPY has been used to couple to drugs but its length of 36 amino acids also implies complex synthesis and high production costs. Therefore, shorter ligands are desirable. However, truncated versions of neuropeptide Y (NPY) usually result in reduced binding, antagonists, or only partial G-protein-biased agonists. Herein, we report on a nonamer peptide derived from the C terminus of NPY that is modified by a carbaborane, which is able to activate hY R fully in terms of G-protein activation but also arrestin recruitment and internalisation. We provide evidence that this unique behaviour is due to the bulky nature of the carbaborane cluster, which might address a specific second binding pocket in hY R that is crucial for arrestin recruitment. Thus, this study helps in deciphering ligand-induced onset of different pathways in hY R mediated signalling.

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Section: Resultsmentioning

confidence: 99%

Section: G-protein Signallingmentioning

confidence: 99%

Carbaboranylation of Truncated C‐Terminal Neuropeptide Y Analogue Leads to Full hY₁ Receptor Agonism

et al. 2018

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“…The N G ‐propionylated argininamide 3 was prepared by propionylation of building block 6 at the guanidine group and subsequent treatment with trifluoroacetic acid (TFA) to remove the N G ‐Boc group (Scheme ). Treatment of amine precursor 8 with succinimidyl propanoate ( 7 ) gave the potential radioligand 4 (Scheme ).…”

Section: Resultsmentioning

confidence: 99%

“…Argininamide 1 was the first highly selective Y 1 R antagonist with an affinity in the single‐digit nanomolar range, and its derivatization led to radio, fluorescent, and bivalent Y 1 R ligands . By contrast, the structurally closely related argininamide BIBO3304 ( 2 ) (Fig.…”

Section: Introductionmentioning

confidence: 99%

“…A) reported to exhibit sub‐nanomolar Y 1 R affinity (IC 50 = 0.38 , K i = 0.25 nM ), has not been exploited for the preparation of pharmacological tools such as radio or fluorescence ligands. Recently, the dimerization of argininamide 2 via spacers attached at the guanidine or the urea moiety yielded bivalent Y 1 R antagonists with markedly lower affinities ( K i 200–330 nM) , suggesting that large substituents are not well tolerated at these positions. In this work, the structure of 2 was modified to explore if propionylation is tolerated and in which position derivatization is most favorable (variants I–III, Fig.…”

Section: Introductionmentioning

confidence: 99%

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Toward Labeled Argininamide‐Type NPY Y₁ Receptor Antagonists: Identification of a Favorable Propionylation Site in BIBO3304

Keller

Schindler

Bernhardt

et al. 2015

Archiv der Pharmazie

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Aiming at molecular tools for the neuropeptide Y Y1 receptor (Y1 R), three types of derivatives of the argininamide-type Y1 R antagonist BIBO3304 were prepared by (i) propionylation at the guanidine group (3), (ii) substitution at the urea moiety with a propionamidobutyl residue (4), and (iii) replacement of ureidomethyl by a propionylaminomethyl group (5). With Ki and Kb values in the range of 1.5-4.3 nM, determined in binding and functional assays, and high selectivity for the Y1 R over the Y2 R, Y4 R, and Y5 R, compounds 4 and 5 were identified as promising candidates for radiolabeling by [(3) H]propionylation according to established protocols.

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Novel composite oxygen‐containing resins with effective adsorption towards anilines: physical & chemical adsorption

Zheng

et al. 2020

J of Chemical Tech & Biotech

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BACKGROUNDThe adsorption resins have been successfully used for the treatment of various types of industrial wastewater due to their excellent advantages of high degree of harmlessness, wonderful resource utilization effect, and adjustable material structure. However, the adsorption capacity of traditional resin to the high polarity aniline has been limited since the adsorption mainly relies on hydrophobic adsorption.RESULTSIn this study, novel oxygen‐containing resins were prepared by modifying a benzene skeleton through chemical functional groups screening and physical structure regulation. The influences of functional groups to the precursor resins were thoroughly studied and the adsorption capacity of the dihydrofuran‐2,5‐dione modified resins was 7.9% higher than the precursor resins, exhibiting the unparalleled adsorption activity to p‐aminobenzoic acid (PABA). Subsequently, a series of dihydrofuran‐2,5‐dione modified crosslinking resins named FSG1‐5 were prepared with various physical structures. The resin FSG‐2 exhibited the best adsorption property, as the adsorption capacity to p‐aminobenzoic acid was 28.3% higher than H‐103 (a commercial hyper‐cross‐linked resin).CONCLUSIONOn the basis of the comparison of kinetics, thermodynamics, and resin's physicochemical structure, FSG‐2 could achieve efficient adsorption to aniline compounds by physical adsorption, such as π‐π conjugation, molecular size effect, and chemical adsorption, including hydrogen bonding and acid–base effect enhanced the adsorption interaction, which laid a theoretical foundation for the design and preparation of new materials. © 2020 Society of Chemical Industry

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Dimeric argininamide-type neuropeptide Y receptor antagonists: Chiral discrimination between Y1 and Y4 receptors

Cited by 18 publications

References 29 publications

Carbaboranylation of Truncated C‐Terminal Neuropeptide Y Analogue Leads to Full hY₁ Receptor Agonism

Carbaboranylation of Truncated C‐Terminal Neuropeptide Y Analogue Leads to Full hY₁ Receptor Agonism

Toward Labeled Argininamide‐Type NPY Y₁ Receptor Antagonists: Identification of a Favorable Propionylation Site in BIBO3304

Novel composite oxygen‐containing resins with effective adsorption towards anilines: physical & chemical adsorption

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Dimeric argininamide-type neuropeptide Y receptor antagonists: Chiral discrimination between Y1 and Y4 receptors

Cited by 18 publications

References 29 publications

Carbaboranylation of Truncated C‐Terminal Neuropeptide Y Analogue Leads to Full hY1 Receptor Agonism

Carbaboranylation of Truncated C‐Terminal Neuropeptide Y Analogue Leads to Full hY1 Receptor Agonism

Toward Labeled Argininamide‐Type NPY Y1 Receptor Antagonists: Identification of a Favorable Propionylation Site in BIBO3304

Novel composite oxygen‐containing resins with effective adsorption towards anilines: physical & chemical adsorption

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Carbaboranylation of Truncated C‐Terminal Neuropeptide Y Analogue Leads to Full hY₁ Receptor Agonism

Carbaboranylation of Truncated C‐Terminal Neuropeptide Y Analogue Leads to Full hY₁ Receptor Agonism

Toward Labeled Argininamide‐Type NPY Y₁ Receptor Antagonists: Identification of a Favorable Propionylation Site in BIBO3304