Showing papers by "Pál Gergely published in 2017"

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Journal Article•DOI•

Nanomolar inhibitors of glycogen phosphorylase based on β-D-glucosaminyl heterocycles: a combined synthetic, enzyme kinetic and protein crystallography study

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Éva Bokor¹, Efthimios Kyriakis², Theodora G.A. Solovou², Csenge Koppány¹, Anastassia L. Kantsadi², Katalin E. Szabó¹, Andrea Szakács¹, Georgios A Stravodimos², Tibor Docsa¹, Vassiliki T. Skamnaki², Spyros E. Zographos, Pál Gergely¹, Demetres D. Leonidas², László Somsák¹ - Show less +10 more•Institutions (2)

University of Debrecen¹, University of Thessaly²

03 Oct 2017-Journal of Medicinal Chemistry

TL;DR: An X-ray crystallography study of the rabbit muscle GPb inhibitor complexes revealed structural features of the strong binding and offered an explanation for the differences in inhibitory potency between glucosyl and glucosaminyl derivatives and also for the Differences between imidazole and 1,2,4-triazole analogues.

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Abstract: Aryl substituted 1-(β-d-glucosaminyl)-1,2,3-triazoles as well as C-β-d-glucosaminyl 1,2,4-triazoles and imidazoles were synthesized and tested as inhibitors against muscle and liver isoforms of glycogen phosphorylase (GP). While the N-β-d-glucosaminyl 1,2,3-triazoles showed weak or no inhibition, the C-β-d-glucosaminyl derivatives had potent activity, and the best inhibitor was the 2-(β-d-glucosaminyl)-4(5)-(2-naphthyl)-imidazole with a Ki value of 143 nM against human liver GPa. An X-ray crystallography study of the rabbit muscle GPb inhibitor complexes revealed structural features of the strong binding and offered an explanation for the differences in inhibitory potency between glucosyl and glucosaminyl derivatives and also for the differences between imidazole and 1,2,4-triazole analogues.

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