Protection of pancreatic islets from oxidative cell death by a peripherally-active morphinan with increased drug safety

Okka Scholz; Elena Huß; Silke Otter; Diran Herebian; Anna Hamacher; Laura Mariana Levy; Stanimira Hristeva; Miguel Sanz; Haresh Ajani; Alfredo Rodriguez Puentes; Torsten Hoffmann; Jens Hogeback; Anke Unger; Susanne Terheyden; Michelle Reina do Fundo; Bedair Dewidar; Michael Roden; Eckhard Lammert

doi:10.1016/j.molmet.2023.101775

Protection of pancreatic islets from oxidative cell death by a peripherally-active morphinan with increased drug safety

Mol Metab. 2023 Sep:75:101775. doi: 10.1016/j.molmet.2023.101775. Epub 2023 Jul 12.

Authors

Okka Scholz¹, Elena Huß¹, Silke Otter¹, Diran Herebian², Anna Hamacher³, Laura Mariana Levy⁴, Stanimira Hristeva⁴, Miguel Sanz⁴, Haresh Ajani⁴, Alfredo Rodriguez Puentes⁴, Torsten Hoffmann⁴, Jens Hogeback⁵, Anke Unger⁶, Susanne Terheyden⁶, Michelle Reina do Fundo⁷, Bedair Dewidar⁷, Michael Roden⁸, Eckhard Lammert⁹

Affiliations

¹ Institute of Metabolic Physiology, Heinrich Heine University, D-40225 Düsseldorf, Germany; Institute for Vascular and Islet Cell Biology, German Diabetes Center (DDZ), Leibniz Center for Diabetes Research at Heinrich Heine University, D-40225 Düsseldorf, Germany; German Center for Diabetes Research (DZD e.V.), Partner Düsseldorf, Neuherberg, D-85764 Neuherberg, Germany.
² Department of General Pediatrics, Neonatology and Pediatric Cardiology, Medical Faculty and University Hospital, Heinrich Heine University, D-40225 Düsseldorf, Germany.
³ Institute of Metabolic Physiology, Heinrich Heine University, D-40225 Düsseldorf, Germany; Institute for Vascular and Islet Cell Biology, German Diabetes Center (DDZ), Leibniz Center for Diabetes Research at Heinrich Heine University, D-40225 Düsseldorf, Germany.
⁴ Taros Chemicals GmbH & Co. KG, D-44227 Dortmund, Germany.
⁵ A&M Labor für Analytik und Metabolismusforschung Service GmbH, D-50126 Bergheim, Germany.
⁶ Lead Discovery Center GmbH & Co. KG, D-44227 Dortmund, Germany.
⁷ German Center for Diabetes Research (DZD e.V.), Partner Düsseldorf, Neuherberg, D-85764 Neuherberg, Germany; Institute for Clinical Diabetology, German Diabetes Center (DDZ), Leibniz Center for Diabetes Research at Heinrich Heine University, D-40225 Düsseldorf, Germany.
⁸ German Center for Diabetes Research (DZD e.V.), Partner Düsseldorf, Neuherberg, D-85764 Neuherberg, Germany; Institute for Clinical Diabetology, German Diabetes Center (DDZ), Leibniz Center for Diabetes Research at Heinrich Heine University, D-40225 Düsseldorf, Germany; Department of Endocrinology and Diabetology, Medical Faculty and University Hospital, Heinrich Heine University, D-40225 Düsseldorf, Germany.
⁹ Institute of Metabolic Physiology, Heinrich Heine University, D-40225 Düsseldorf, Germany; Institute for Vascular and Islet Cell Biology, German Diabetes Center (DDZ), Leibniz Center for Diabetes Research at Heinrich Heine University, D-40225 Düsseldorf, Germany; German Center for Diabetes Research (DZD e.V.), Partner Düsseldorf, Neuherberg, D-85764 Neuherberg, Germany. Electronic address: lammert@hhu.de.

Abstract

Objective: Dextromethorphan (DXM) is a commonly used antitussive medication with positive effects in people with type 2 diabetes mellitus, since it increases glucose tolerance and protects pancreatic islets from cell death. However, its use as an antidiabetic medication is limited due to its central nervous side effects and potential use as a recreational drug. Therefore, we recently modified DXM chemically to reduce its blood-brain barrier (BBB) penetration and central side effects. However, our best compound interacted with the cardiac potassium channel hERG (human ether-à-go-go-related gene product) and the μ-opioid receptor (MOR). Thus, the goal of this study was to reduce the interaction of our compound with these targets, while maintaining its beneficial properties.

Methods: Receptor and channel binding assays were conducted to evaluate the drug safety of our DXM derivative. Pancreatic islets were used to investigate the effect of the compound on insulin secretion and islet cell survival. Via liquor collection from the brain and a behavioral assay, we analyzed the BBB permeability. By performing intraperitoneal and oral glucose tolerance tests as well as pharmacokinetic analyses, the antidiabetic potential and elimination half-life were investigated, respectively. To analyze the islet cell-protective effect, we used fluorescence microscopy as well as flow cytometric analyses.

Results: Here, we report the design and synthesis of an optimized, orally available BBB-impermeable DXM derivative with lesser binding to hERG and MOR than previous ones. We also show that the new compound substantially enhances glucose-stimulated insulin secretion (GSIS) from mouse and human islets and glucose tolerance in mice as well as protects pancreatic islets from cell death induced by reactive oxygen species and that it amplifies the effects of tirzepatide on GSIS and islet cell viability.

Conclusions: We succeeded to design and synthesize a novel morphinan derivative that is BBB-impermeable, glucose-lowering and islet cell-protective and has good drug safety despite its morphinan and imidazole structures.

Keywords: Blood–brain barrier; Dextromethorphan; Diabetes mellitus; Drug discovery; Pancreatic islet cell protection; Pancreatic islets.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Diabetes Mellitus, Type 2* / metabolism
Glucose / metabolism
Humans
Hypoglycemic Agents / pharmacology
Insulin / metabolism
Islets of Langerhans* / metabolism
Mice
Morphinans* / metabolism
Morphinans* / pharmacology
Oxidative Stress

Substances

Insulin
Morphinans
Glucose
Hypoglycemic Agents