Literature DB >> 26108304

A comprehensive review of the pharmacodynamics of the SGLT2 inhibitor empagliflozin in animals and humans.

Martin C Michel1, Eric Mayoux, Volker Vallon.   

Abstract

Empagliflozin (formerly known as BI 10773) is a potent, competitive, and selective inhibitor of the sodium glucose transporter SGLT2, which mediates glucose reabsorption in the early proximal tubule and most of the glucose reabsorption by the kidney, overall. Accordingly, empagliflozin treatment increased urinary glucose excretion. This has been observed across multiple species including humans and was reported under euglycemic conditions, in obesity and, most importantly, in type 2 diabetic patients and multiple animal models of type 2 diabetes and of type 1 diabetes. This led to a reduction in blood glucose, smaller blood glucose excursions during oral glucose tolerance tests, and, upon chronic treatment, a reduction in HbA1c in animal models and patients. In rodents, such effects were observed in early and late phases of experimental diabetes and were associated with preservation of pancreatic β-cell function. Combination studies in animals demonstrated that beneficial metabolic effects of empagliflozin may also manifest when added to other types of anti-hyperglycemic treatments including linagliptin and pioglitazone. While some anti-hyperglycemic drugs lead to weight gain, empagliflozin treatment was associated with reduced body weight in normoglycemic obese and non-obese animals despite an increased food intake, largely due to a loss of adipose tissue; on the other hand, empagliflozin preserved body weight in models of type 1 diabetes. Empagliflozin improved endothelial dysfunction in diabetic rats and arterial stiffness, reduced blood pressure in diabetic patients, and attenuated early signs of nephropathy in diabetic animal models. Taken together, the SGLT2 inhibitor empagliflozin improves glucose metabolism by enhancing urinary glucose excretion; upon chronic administration, at least in animal models, the reductions in blood glucose levels are associated with beneficial effects on cardiovascular and renal complications of diabetes.

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Year:  2015        PMID: 26108304      PMCID: PMC5896322          DOI: 10.1007/s00210-015-1134-1

Source DB:  PubMed          Journal:  Naunyn Schmiedebergs Arch Pharmacol        ISSN: 0028-1298            Impact factor:   3.000


  64 in total

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Journal:  Am J Physiol Endocrinol Metab       Date:  2012-11-13       Impact factor: 4.310

Review 4.  Biology of human sodium glucose transporters.

Authors:  Ernest M Wright; Donald D F Loo; Bruce A Hirayama
Journal:  Physiol Rev       Date:  2011-04       Impact factor: 37.312

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Journal:  Diabetes       Date:  2008-03-20       Impact factor: 9.461

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Journal:  Diabetes       Date:  2011-11-28       Impact factor: 9.461

10.  Pharmacokinetic and pharmacodynamic profile of empagliflozin, a sodium glucose co-transporter 2 inhibitor.

Authors:  André J Scheen
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  19 in total

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2.  Preclinical research strategies for newly approved drugs as reflected in early publication patterns.

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5.  Sodium-Glucose Cotransporter 2 Inhibitor and a Low Carbohydrate Diet Affect Gluconeogenesis and Glycogen Content Differently in the Kidney and the Liver of Non-Diabetic Mice.

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Journal:  Cardiovasc Diabetol       Date:  2019-02-07       Impact factor: 9.951

8.  Safety, tolerability and effects on cardiometabolic risk factors of empagliflozin monotherapy in drug-naïve patients with type 2 diabetes: a double-blind extension of a Phase III randomized controlled trial.

Authors:  Michael Roden; Ludwig Merker; Anita Vedel Christiansen; Flavien Roux; Afshin Salsali; Gabriel Kim; Peter Stella; Hans J Woerle; Uli C Broedl
Journal:  Cardiovasc Diabetol       Date:  2015-12-23       Impact factor: 9.951

Review 9.  Cardiovascular Effects of New Oral Glucose-Lowering Agents: DPP-4 and SGLT-2 Inhibitors.

Authors:  André J Scheen
Journal:  Circ Res       Date:  2018-05-11       Impact factor: 17.367

Review 10.  Sodium-glucose cotransporters: Functional properties and pharmaceutical potential.

Authors:  Ryuhei Sano; Yuichi Shinozaki; Takeshi Ohta
Journal:  J Diabetes Investig       Date:  2020-04-16       Impact factor: 4.232

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