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11-Aminostrychnine and N-(Strychnine-11-yl)propionamide: Synthesis, Configuration, and Pharmacological Evaluation at Glycine Receptors.

Darius P ZlotosAmal M Y MohsenYasmine M MandourMohamed A MarzoukUlrike BreitingerCarmen VillmannHans-Georg BreitingerChristoph A SotrifferAnders A JensenGerhard Bringmann
Published in: Journal of natural products (2019)
(11S)-11-Aminostrychnine (1) and N-[(11S)-strychnine-11-yl]propionamide (2) were synthesized and characterized as antagonists of homomeric α1 and heteromeric α1β glycine receptors in a functional fluorescence-based assay and a patch-clamp assay and in radioligand binding studies. The absolute configuration at C-11 of 1 was determined based on vicinal coupling constants and NOESY data. Docking experiments to the orthosteric binding site of the α3 glycine receptor showed a binding mode of compound 2 analogous to that of strychnine, explaining its high antagonistic potency. The findings identify the C-11 amide function of strychnine as a suitable linker group for the future development of dimeric strychnine analogues targeting glycine receptors. The findings extend the SAR of strychnine at glycine receptors.
Keyphrases
  • high throughput
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  • molecular dynamics
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  • dna binding
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  • single molecule
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  • current status
  • protein protein
  • energy transfer