Effects of neprilysin and neprilysin inhibitors on glucose homeostasis: Controversial points and a promising arena

Author:

AlAnazi Faisal Holil1,Al‐kuraishy Hayder M.2,Al‐Gareeb Ali I.2,Alexiou Athanasios34,Papadakis Marios5,Ogaly Hanan A.6ORCID,Alanazi Yousef Abud7ORCID,Saad Hebatallah M.8ORCID,Batiha Gaber El‐Saber9

Affiliation:

1. Department of Medicine, College of Medicine Majmaah University Majmaah Saudi Arabia

2. Department of Clinical Pharmacology and Medicine, College of Medicine ALmustansiriyia University Baghdad Iraq

3. Department of Science and Engineering Novel Global Community Educational Foundation Hebersham New South Wales Australia

4. AFNP Med Wien Austria

5. Department of Surgery II University Hospital Witten‐Herdecke, University of Witten‐Herdecke Wuppertal Germany

6. Chemistry Department, College of Science King Khalid University Abha Saudi Arabia

7. Department of Pediatrics, College of Medicine Majmaah University Majmaah Saudi Arabia

8. Department of Pathology, Faculty of Veterinary Medicine Matrouh University Marsa Matruh Egypt

9. Department of Pharmacology and Therapeutics, Faculty of Veterinary Medicine Damanhour University Damanhour Egypt

Abstract

AbstractNeprilysin (NEP) is a transmembrane zinc‐dependent metalloproteinase that inactivates various peptide hormones including glucagon‐like peptide 1 (GLP‐1). NEP inhibitors may be effective in the management of type 2 diabetes mellitus (T2DM) by increasing the circulating level of GLP‐1. However, acute‐effect NEP inhibitors may lead to detrimental effects by increasing blood glucose independent of GLP‐1. These findings suggest a controversial point regarding the potential role of NEP inhibitors on glucose homeostasis in T2DM patients. Therefore, this perspective aimed to clarify the controversial points concerning the role of NEP inhibitors on glucose homeostasis in T2DM. NEP inhibitors may lead to beneficial effects by inhibition of NEP, which is involved in the impairment of glucose homeostasis through modulation of insulin resistance. NEP increases dipeptidyl peptidase‐4 (DPP4) activity and contributes to increasing active GLP‐1 proteolysis so NEP inhibitors may improve glycemic control through increasing endogenous GLP‐1 activity and reduction of DPP4 activity. Thus, NEP inhibitors could be effective alone or in combination with antidiabetic agents in treating T2DM patients. However, long‐term and short‐term effects of NEP inhibitors may lead to a detrimental effect on insulin sensitivity and glucose homeostasis through different mechanisms including augmentation of substrates and pancreatic amyloid deposition. These findings are confirmed in animal but not in humans. In conclusion, NEP inhibitors produce beneficial rather than detrimental effects on glucose homeostasis and insulin sensitivity in humans though most of the detrimental effects of NEP inhibitors are confirmed in animal studies.

Publisher

Wiley

Subject

Endocrinology, Diabetes and Metabolism

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