Sabine Kerres scite author profile

An efficient method for the synthesis of substituted cyclobutanes from cinnamates, chalcones, and styrenes has been developed utilizing a visible-light triplet sensitisation mode. This reaction provides a diverse range of substituted cyclobutanes in high yields under mild conditions without the need of external additives. Good regioselectivity is obtained due to strong π-π-stacking of arene moieties, whereas diastereoselectivity relies on the electronic effects or ortho-substitution of the arene substrate. The utility of this transformation is demonstrated by the formal synthesis of the lignane natural product (±)-Tanegool.

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Asymmetric Synthesis of Both Enantiomers of Arteludovicinolide A

Kreuzer

Kerres

Ertl

et al. 2013

Org. Lett.

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The first total synthesis of either enantiomer of Arteludovicinolide A and their biological evaluation is reported, featuring a new strategy for the asymmetric construction of γ-butyrolactones with stereogenic side chains in the 4-position. Starting from the renewable resource methyl 2-furoate, the sesquiterpene lactone was synthesized in 9 steps and 4.8% overall yield via an asymmetric cyclopropanation and two diastereoselective nucleophile additions making use of a donor-acceptor-cyclopropane-lactonization cascade. At noncytotoxic concentrations (≤10 μM) (+)-1 was found to have a 15 times higher anti-inflammatory activity (4.87 ± 1.1 μM) than previously reported for concentrations of ≥45 μM.

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Visible Light‐Mediated Synthesis of Enantiopure γ‐Cyclobutane Amino and 3‐(Aminomethyl)‐5‐phenylpentanoic Acids

et al. 2019

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A visible light-mediated [2 + 2] photocycloaddition of amide-linked dienes using [Ir(dtbbpy)(dF(CF 3 )ppy) 2 ]PF 6 as triplet sensitizer was applied to generate a variety of N-tert-butyl, Nbenzyl-and N-tert-butoxycarbonyl-protected 3-azabicyclo[3.2.0]heptan-2-ones in good yields and with good diastereoselectivity. Density functional theory calculations shed light on the conformational prerequisites for the [2 + 2] photocycloaddition. The bicyclic key structures could be readily transformed into g-cyclobutane amino acids. For the obtained racemic 3-phenyl-2-aminocyclobutane-1-carboxylic acid the resolution with chiral oxazolidin-2-one is demonstrated to allow access to both enantiomers. Alternatively, a chiral auxiliary approach led as well to the enantiomerically pure target compound. Finally, the synthesis of either enantiomer of 3-(aminomethyl)-5-phenylpentanoic acid, the racemate being described as an anticonvulsant, is described.

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Stereochemistry-Driven Interactions of α,γ-Peptide Ligands with the Neuropeptide Y Y₄-Receptor

et al. 2023

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The G-protein-coupled Y 4 -receptor (Y 4 R) and its endogenous ligand, pancreatic polypeptide (PP), suppress appetite in response to food intake and, thus, are attractive drug targets for body-weight control. The Cterminus of human PP (hPP), T 32 -R 33 -P 34 -R 35 -Y 36 -NH 2 , penetrates deep into the binding pocket with its tyrosine-amide and di-arginine motif. Here, we present two C-terminally amidated α,γ-hexapeptides (1a/b) with sequence Ac-R 31 -γ-CBAA 32 -R 33 -L 34 -R 35 -Y 36 -NH 2 , where γ-CBAA is the (1R,2S,3R)configured 2-(aminomethyl)-3-phenylcyclobutanecarboxyl moiety (1a) or its mirror image (1b). Both peptides bind the Y 4 R (K i of 1a/b: 0.66/12 nM) and act as partial agonists (intrinsic activity of 1a/b: 50/39%). Their induced-fit binding poses in the Y 4 R pocket are unique and build ligand− receptor contacts distinct from those of the C-terminus of the endogenous ligand hPP. We conclude that energetically favorable interactions, although they do not match those of the native ligand hPP, still guarantee high binding affinity (with 1a rivaling hPP) but not the maximum receptor activation.

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Sabine Kerres

Photosensitised regioselective [2+2]-cycloaddition of cinnamates and related alkenes

Asymmetric Synthesis of Both Enantiomers of Arteludovicinolide A

Visible Light‐Mediated Synthesis of Enantiopure γ‐Cyclobutane Amino and 3‐(Aminomethyl)‐5‐phenylpentanoic Acids

Stereochemistry-Driven Interactions of α,γ-Peptide Ligands with the Neuropeptide Y Y₄-Receptor

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About

Sabine Kerres

Photosensitised regioselective [2+2]-cycloaddition of cinnamates and related alkenes

Asymmetric Synthesis of Both Enantiomers of Arteludovicinolide A

Visible Light‐Mediated Synthesis of Enantiopure γ‐Cyclobutane Amino and 3‐(Aminomethyl)‐5‐phenylpentanoic Acids

Stereochemistry-Driven Interactions of α,γ-Peptide Ligands with the Neuropeptide Y Y4-Receptor

Contact Info

Product

Resources

About

Stereochemistry-Driven Interactions of α,γ-Peptide Ligands with the Neuropeptide Y Y₄-Receptor