Imeglimin preserves islet β‐cell mass in Type 2 diabetic ZDF rats

Imeglimin preserves islet β‐cell mass in Type 2 diabetic ZDF rats

Abstract Objectives Type 2 diabetes (T2D) is driven by progressive dysfunction and loss of pancreatic β‐cell mass. Imeglimin is a first‐in‐class novel drug candidate that improves glycaemia and glucose‐stimulated insulin secretion in preclinical models and patients. Given evidence that imeglimin can...

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Main Authors: Sophie Hallakou‐Bozec, Micheline Kergoat, David E. Moller, Sébastien Bolze
Format: Article
Language:English
Published: Wiley 2021-04-01
Series:Endocrinology, Diabetes & Metabolism
Subjects:
animal models
islet
imeglimin
new therapies
Online Access:https://doi.org/10.1002/edm2.193
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spelling doaj-ec2f8968c9224c7d8f8517a289f21de62021-04-08T13:20:50ZengWileyEndocrinology, Diabetes & Metabolism2398-92382021-04-0142n/an/a10.1002/edm2.193Imeglimin preserves islet β‐cell mass in Type 2 diabetic ZDF ratsSophie Hallakou‐Bozec0Micheline Kergoat1David E. Moller2Sébastien Bolze3Poxel SA Lyon FranceMetabrain Research Maisons‐Alfort FrancePoxel SA Lyon FrancePoxel SA Lyon FranceAbstract Objectives Type 2 diabetes (T2D) is driven by progressive dysfunction and loss of pancreatic β‐cell mass. Imeglimin is a first‐in‐class novel drug candidate that improves glycaemia and glucose‐stimulated insulin secretion in preclinical models and patients. Given evidence that imeglimin can attenuate β‐cell dysfunction and protect β cells in vitro, we postulated that imeglimin could also exert longer term effects to prevent pancreatic β‐cell death and preserve functional β‐cell mass in vivo. Methods Zucker diabetic fatty (ZDF) male rats were treated by oral gavage with imeglimin at a standard dose of 150 mg/kg or vehicle, twice daily for five weeks. At treatment completion, oral glucose tolerance tests were performed in fasted animals before a thorough histomorphometry and immunohistochemical analysis was conducted on pancreas tissue slices to assess cellular composition and disease status. Results Imeglimin treatment significantly improved glucose‐stimulated insulin secretion (augmentation of the insulinogenic index) and improved glycaemia. Both basal insulinaemia and pancreatic insulin content were also increased by imeglimin. In ZDF control rats, islet structure was disordered with few β‐cells; after imeglimin treatment, islets appeared healthier with more normal morphology in association with a significant increase in insulin‐positive β‐cells. The increase in β‐cell mass was associated with a greater degree of β‐cell proliferation in the presence of reduced apoptosis. Unexpectedly, a decrease in as a α‐cell mass was also documented due to an apparent antiproliferative effect of imeglimin on this cell type. Conclusion In male ZDF rats, chronic imeglimin treatment corrects a paramount component of type 2 diabetes progression: progressive loss of functional β‐cell mass. In addition, imeglimin may also moderate a‐cell turnover to further ameliorate hyperglycaemia. Cumulatively, these cellular effects suggest that imeglimin may provide for disease modifying effects to preserve functional β‐cell mass.https://doi.org/10.1002/edm2.193animal modelsisletimegliminnew therapies
collection DOAJ
language English
format Article
sources DOAJ
author Sophie Hallakou‐Bozec
Micheline Kergoat
David E. Moller
Sébastien Bolze
spellingShingle Sophie Hallakou‐Bozec
Micheline Kergoat
David E. Moller
Sébastien Bolze
Imeglimin preserves islet β‐cell mass in Type 2 diabetic ZDF rats
Endocrinology, Diabetes & Metabolism
animal models
islet
imeglimin
new therapies
author_facet Sophie Hallakou‐Bozec
Micheline Kergoat
David E. Moller
Sébastien Bolze
author_sort Sophie Hallakou‐Bozec
title Imeglimin preserves islet β‐cell mass in Type 2 diabetic ZDF rats
title_short Imeglimin preserves islet β‐cell mass in Type 2 diabetic ZDF rats
title_full Imeglimin preserves islet β‐cell mass in Type 2 diabetic ZDF rats
title_fullStr Imeglimin preserves islet β‐cell mass in Type 2 diabetic ZDF rats
title_full_unstemmed Imeglimin preserves islet β‐cell mass in Type 2 diabetic ZDF rats
title_sort imeglimin preserves islet β‐cell mass in type 2 diabetic zdf rats
publisher Wiley
series Endocrinology, Diabetes & Metabolism
issn 2398-9238
publishDate 2021-04-01
description Abstract Objectives Type 2 diabetes (T2D) is driven by progressive dysfunction and loss of pancreatic β‐cell mass. Imeglimin is a first‐in‐class novel drug candidate that improves glycaemia and glucose‐stimulated insulin secretion in preclinical models and patients. Given evidence that imeglimin can attenuate β‐cell dysfunction and protect β cells in vitro, we postulated that imeglimin could also exert longer term effects to prevent pancreatic β‐cell death and preserve functional β‐cell mass in vivo. Methods Zucker diabetic fatty (ZDF) male rats were treated by oral gavage with imeglimin at a standard dose of 150 mg/kg or vehicle, twice daily for five weeks. At treatment completion, oral glucose tolerance tests were performed in fasted animals before a thorough histomorphometry and immunohistochemical analysis was conducted on pancreas tissue slices to assess cellular composition and disease status. Results Imeglimin treatment significantly improved glucose‐stimulated insulin secretion (augmentation of the insulinogenic index) and improved glycaemia. Both basal insulinaemia and pancreatic insulin content were also increased by imeglimin. In ZDF control rats, islet structure was disordered with few β‐cells; after imeglimin treatment, islets appeared healthier with more normal morphology in association with a significant increase in insulin‐positive β‐cells. The increase in β‐cell mass was associated with a greater degree of β‐cell proliferation in the presence of reduced apoptosis. Unexpectedly, a decrease in as a α‐cell mass was also documented due to an apparent antiproliferative effect of imeglimin on this cell type. Conclusion In male ZDF rats, chronic imeglimin treatment corrects a paramount component of type 2 diabetes progression: progressive loss of functional β‐cell mass. In addition, imeglimin may also moderate a‐cell turnover to further ameliorate hyperglycaemia. Cumulatively, these cellular effects suggest that imeglimin may provide for disease modifying effects to preserve functional β‐cell mass.
topic animal models
islet
imeglimin
new therapies
url https://doi.org/10.1002/edm2.193
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AT michelinekergoat imegliminpreservesisletbcellmassintype2diabeticzdfrats
AT davidemoller imegliminpreservesisletbcellmassintype2diabeticzdfrats
AT sebastienbolze imegliminpreservesisletbcellmassintype2diabeticzdfrats
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