Literature DB >> 30017776

SGLT2 inhibition and glucagon secretion in humans.

C Saponaro1, F Pattou2, C Bonner3.   

Abstract

With the increasing prevalence of type 2 diabetes (T2D), therapies aimed at delineating diabetes pathophysiology and understanding their mechanisms of action are of critical importance. As such, growing interest in the clinical pharmacology of sodium-glucose cotransporter 2 (SGLT2) and its inhibition by gliflozins in the treatment of T2D is becoming increasingly evident. SGLT2 inhibition results in urinary glucose excretion, thereby reducing blood glucose levels. The importance of this homoeostasis mechanism is evident from several clinical trials demonstrating that patients taking this class of compounds have reductions in glycaemia, body weight and blood pressure compared with other antidiabetic agents. Yet, while such outcomes are very encouraging, some studies have reported elevated plasma glucagon levels and endogenous glucose production (EGP), two traits that are already prevalent in T2D. However, these findings were later explained by the specific expression of SGLT2 by pancreatic alpha cells, where glucagon secretion is directly regulated. Although conflicting data are now emerging on SGLT2 regulation of glucagon secretion, as SGLT2 is not expressed in the intestines, circulating glucagon concentrations are most likely of pancreatic origin. Thus, the present review considers the mechanism of action of SGLT2 inhibitors in the regulation of glucagon secretion, and the discrepancies in data from mice compared with people. The pragmatic use of human islets to accurately decipher SGLT2 inhibition in the regulation of glucagon secretion is also discussed.
Copyright © 2018. Published by Elsevier Masson SAS.

Entities:  

Keywords:  Glucagon secretion; SGLT2 inhibition

Mesh:

Substances:

Year:  2018        PMID: 30017776     DOI: 10.1016/j.diabet.2018.06.005

Source DB:  PubMed          Journal:  Diabetes Metab        ISSN: 1262-3636            Impact factor:   6.041


  9 in total

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Review 2.  SGLT2 inhibitors: a focus on cardiac benefits and potential mechanisms.

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Review 4.  SGLT2 Inhibitors: A Review of Their Antidiabetic and Cardioprotective Effects.

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Review 5.  Sodium-glucose cotransporter 2 inhibition: towards an indication to treat diabetic kidney disease.

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6.  Sodium-glucose cotransporter 2 inhibition does not reduce hepatic steatosis in overweight, insulin-resistant patients without type 2 diabetes.

Authors:  Thomas Marjot; Charlotte J Green; Catriona A Charlton; Thomas Cornfield; Jonathan Hazlehurst; Ahmad Moolla; Sarah White; Jane Francis; Stefan Neubauer; Jeremy Fl Cobbold; Leanne Hodson; Jeremy W Tomlinson
Journal:  JGH Open       Date:  2019-11-05

7.  SGLT2 is not expressed in pancreatic α- and β-cells, and its inhibition does not directly affect glucagon and insulin secretion in rodents and humans.

Authors:  Heeyoung Chae; Robert Augustin; Eva Gatineau; Eric Mayoux; Mohammed Bensellam; Nancy Antoine; Firas Khattab; Bao-Khanh Lai; Davide Brusa; Birgit Stierstorfer; Holger Klein; Bilal Singh; Lucie Ruiz; Michael Pieper; Michael Mark; Pedro L Herrera; Fiona M Gribble; Frank Reimann; Anne Wojtusciszyn; Christophe Broca; Nano Rita; Lorenzo Piemonti; Patrick Gilon
Journal:  Mol Metab       Date:  2020-09-05       Impact factor: 7.422

8.  SGLT2 Inhibitors for Treatment of Refractory Hypomagnesemia: A Case Report of 3 Patients.

Authors:  Evan C Ray; Cary R Boyd-Shiwarski; Pengfei Liu; Danica Novacic; David Cassiman
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9.  The Role of Glucagon in the Acute Therapeutic Effects of SGLT2 Inhibition.

Authors:  Sofie Hædersdal; Asger Lund; Elisabeth Nielsen-Hannerup; Henrik Maagensen; Gerrit van Hall; Jens J Holst; Filip K Knop; Tina Vilsbøll
Journal:  Diabetes       Date:  2020-10-01       Impact factor: 9.337

  9 in total

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