55P0110, a Novel Synthetic Compound Developed from a Plant Derived Backbone Structure, Shows Promising Anti-Hyperglycaemic Activity in Mice

Starting off with a structure derived from the natural compound multiflorine, a derivatisation program aimed at the discovery and initial characterisation of novel compounds with antidiabetic potential. Design and discovery of the structures was guided by oral bioactivities obtained in oral glucose...

Descripción completa

Detalles Bibliográficos
Autores principales: Brunmair, Barbara, Lehner, Zsuzsanna, Stadlbauer, Karin, Adorjan, Immanuel, Frobel, Klaus, Scherer, Thomas, Luger, Anton, Bauer, Leonhardt, Fürnsinn, Clemens
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4431753/
https://www.ncbi.nlm.nih.gov/pubmed/25973898
http://dx.doi.org/10.1371/journal.pone.0126847
_version_ 1782371402207199232
author Brunmair, Barbara
Lehner, Zsuzsanna
Stadlbauer, Karin
Adorjan, Immanuel
Frobel, Klaus
Scherer, Thomas
Luger, Anton
Bauer, Leonhardt
Fürnsinn, Clemens
author_facet Brunmair, Barbara
Lehner, Zsuzsanna
Stadlbauer, Karin
Adorjan, Immanuel
Frobel, Klaus
Scherer, Thomas
Luger, Anton
Bauer, Leonhardt
Fürnsinn, Clemens
author_sort Brunmair, Barbara
collection PubMed
description Starting off with a structure derived from the natural compound multiflorine, a derivatisation program aimed at the discovery and initial characterisation of novel compounds with antidiabetic potential. Design and discovery of the structures was guided by oral bioactivities obtained in oral glucose tolerance tests in mice. 55P0110, one among several new compounds with distinct anti-hyperglycaemic activity, was further examined to characterise its pharmacology and mode of action. Whereas a single oral dose of 55P0110 did not affect basal glycaemia, it markedly improved the glucose tolerance of healthy and diabetic mice (peak blood glucose in glucose tolerance test, mmol/l: healthy mice with 90 mg/kg 55P0110, 17.0±1.2 vs. 10.1±1.1; diabetic mice with 180 mg/kg 55P0110, 23.1±0.9 vs. 11.1±1.4; p<0.001 each). Closer examination argued against retarded glucose resorption from the gut, increased glucose excretion in urine, acute insulin-like or insulin sensitising properties, and direct inhibition of dipeptidyl peptidase-4 as the cause of glucose lowering. Hence, 55P0110 seems to act via a target not exploited by any drug presently approved for the treatment of diabetes mellitus. Whereas the insulinotropic sulfonylurea gliclazide (16 mg/kg) distinctly increased the circulating insulin-per-glucose ratio under basal conditions, 55P0110 (90 mg/kg) lacked such an effect (30 min. after dosing, nmol/mol: vehicle, 2.49±0.27; 55P0110, 2.99±0.35; gliclazide, 8.97±0.49; p<0.001 each vs. gliclazide). Under an exogenous glucose challenge, however, 55P0110 increased this ratio to the same extent as gliclazide (20 min. after glucose feeding: vehicle, 2.53±0.41; 55P0110, 3.80±0.46; gliclazide, 3.99±0.26; p<0.05 each vs. vehicle). By augmenting the glucose stimulated increase in plasma insulin, 55P0110 thus shows distinct anti-hyperglycaemic action in combination with low risk for fasting hypoglycaemia in mice. In summary, we have discovered a novel class of fully synthetic substituted quinazolidines with an attractive pharmacological profile that recommends the structures for further evaluation as candidates for the treatment of diabetes mellitus.
format Online
Article
Text
id pubmed-4431753
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-44317532015-05-27 55P0110, a Novel Synthetic Compound Developed from a Plant Derived Backbone Structure, Shows Promising Anti-Hyperglycaemic Activity in Mice Brunmair, Barbara Lehner, Zsuzsanna Stadlbauer, Karin Adorjan, Immanuel Frobel, Klaus Scherer, Thomas Luger, Anton Bauer, Leonhardt Fürnsinn, Clemens PLoS One Research Article Starting off with a structure derived from the natural compound multiflorine, a derivatisation program aimed at the discovery and initial characterisation of novel compounds with antidiabetic potential. Design and discovery of the structures was guided by oral bioactivities obtained in oral glucose tolerance tests in mice. 55P0110, one among several new compounds with distinct anti-hyperglycaemic activity, was further examined to characterise its pharmacology and mode of action. Whereas a single oral dose of 55P0110 did not affect basal glycaemia, it markedly improved the glucose tolerance of healthy and diabetic mice (peak blood glucose in glucose tolerance test, mmol/l: healthy mice with 90 mg/kg 55P0110, 17.0±1.2 vs. 10.1±1.1; diabetic mice with 180 mg/kg 55P0110, 23.1±0.9 vs. 11.1±1.4; p<0.001 each). Closer examination argued against retarded glucose resorption from the gut, increased glucose excretion in urine, acute insulin-like or insulin sensitising properties, and direct inhibition of dipeptidyl peptidase-4 as the cause of glucose lowering. Hence, 55P0110 seems to act via a target not exploited by any drug presently approved for the treatment of diabetes mellitus. Whereas the insulinotropic sulfonylurea gliclazide (16 mg/kg) distinctly increased the circulating insulin-per-glucose ratio under basal conditions, 55P0110 (90 mg/kg) lacked such an effect (30 min. after dosing, nmol/mol: vehicle, 2.49±0.27; 55P0110, 2.99±0.35; gliclazide, 8.97±0.49; p<0.001 each vs. gliclazide). Under an exogenous glucose challenge, however, 55P0110 increased this ratio to the same extent as gliclazide (20 min. after glucose feeding: vehicle, 2.53±0.41; 55P0110, 3.80±0.46; gliclazide, 3.99±0.26; p<0.05 each vs. vehicle). By augmenting the glucose stimulated increase in plasma insulin, 55P0110 thus shows distinct anti-hyperglycaemic action in combination with low risk for fasting hypoglycaemia in mice. In summary, we have discovered a novel class of fully synthetic substituted quinazolidines with an attractive pharmacological profile that recommends the structures for further evaluation as candidates for the treatment of diabetes mellitus. Public Library of Science 2015-05-14 /pmc/articles/PMC4431753/ /pubmed/25973898 http://dx.doi.org/10.1371/journal.pone.0126847 Text en © 2015 Brunmair et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Brunmair, Barbara
Lehner, Zsuzsanna
Stadlbauer, Karin
Adorjan, Immanuel
Frobel, Klaus
Scherer, Thomas
Luger, Anton
Bauer, Leonhardt
Fürnsinn, Clemens
55P0110, a Novel Synthetic Compound Developed from a Plant Derived Backbone Structure, Shows Promising Anti-Hyperglycaemic Activity in Mice
title 55P0110, a Novel Synthetic Compound Developed from a Plant Derived Backbone Structure, Shows Promising Anti-Hyperglycaemic Activity in Mice
title_full 55P0110, a Novel Synthetic Compound Developed from a Plant Derived Backbone Structure, Shows Promising Anti-Hyperglycaemic Activity in Mice
title_fullStr 55P0110, a Novel Synthetic Compound Developed from a Plant Derived Backbone Structure, Shows Promising Anti-Hyperglycaemic Activity in Mice
title_full_unstemmed 55P0110, a Novel Synthetic Compound Developed from a Plant Derived Backbone Structure, Shows Promising Anti-Hyperglycaemic Activity in Mice
title_short 55P0110, a Novel Synthetic Compound Developed from a Plant Derived Backbone Structure, Shows Promising Anti-Hyperglycaemic Activity in Mice
title_sort 55p0110, a novel synthetic compound developed from a plant derived backbone structure, shows promising anti-hyperglycaemic activity in mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4431753/
https://www.ncbi.nlm.nih.gov/pubmed/25973898
http://dx.doi.org/10.1371/journal.pone.0126847
work_keys_str_mv AT brunmairbarbara 55p0110anovelsyntheticcompounddevelopedfromaplantderivedbackbonestructureshowspromisingantihyperglycaemicactivityinmice
AT lehnerzsuzsanna 55p0110anovelsyntheticcompounddevelopedfromaplantderivedbackbonestructureshowspromisingantihyperglycaemicactivityinmice
AT stadlbauerkarin 55p0110anovelsyntheticcompounddevelopedfromaplantderivedbackbonestructureshowspromisingantihyperglycaemicactivityinmice
AT adorjanimmanuel 55p0110anovelsyntheticcompounddevelopedfromaplantderivedbackbonestructureshowspromisingantihyperglycaemicactivityinmice
AT frobelklaus 55p0110anovelsyntheticcompounddevelopedfromaplantderivedbackbonestructureshowspromisingantihyperglycaemicactivityinmice
AT schererthomas 55p0110anovelsyntheticcompounddevelopedfromaplantderivedbackbonestructureshowspromisingantihyperglycaemicactivityinmice
AT lugeranton 55p0110anovelsyntheticcompounddevelopedfromaplantderivedbackbonestructureshowspromisingantihyperglycaemicactivityinmice
AT bauerleonhardt 55p0110anovelsyntheticcompounddevelopedfromaplantderivedbackbonestructureshowspromisingantihyperglycaemicactivityinmice
AT furnsinnclemens 55p0110anovelsyntheticcompounddevelopedfromaplantderivedbackbonestructureshowspromisingantihyperglycaemicactivityinmice

Ejemplares similares