Evaluating the effectiveness of a novel somatostatin receptor 2 antagonist, ZT-01, for hypoglycemia prevention in a rodent model of type 2 diabetes

Ninoschka C D'Souza; Julian A Aiken; Emily G Hoffman; Sara C Atherley; Sabrina Champsi; Nadia Aleali; Dorsa Shakeri; Maya El-Zahed; Nicky Akbarian; Mehran Nejad-Mansouri; Parinaz Z Bavani; Richard L Liggins; Owen Chan; Michael C Riddell

doi:10.3389/fphar.2024.1302015

Evaluating the effectiveness of a novel somatostatin receptor 2 antagonist, ZT-01, for hypoglycemia prevention in a rodent model of type 2 diabetes

Front Pharmacol. 2024 Feb 28:15:1302015. doi: 10.3389/fphar.2024.1302015. eCollection 2024.

Affiliations

¹ School of Kinesiology and Health Science, York University, Toronto, ON, Canada.
² Zucara Therapeutics, Vancouver, BC, Canada.
³ Department of Internal Medicine, Division of Endocrinology, University of Utah, Salt LakeCity, UT, United States.

Abstract

Background: Elevated levels of somatostatin blunt glucagon counterregulation during hypoglycemia in type 1 diabetes (T1D) and this can be improved using somatostatin receptor 2 (SSTR2) antagonists. Hypoglycemia also occurs in late-stage type 2 diabetes (T2D), particularly when insulin therapy is initiated, but the utility of SSTR2 antagonists in ameliorating hypoglycemia in this disease state is unknown. We examined the efficacy of a single-dose of SSTR2 antagonists in a rodent model of T2D. Methods: High-fat fed (HFF), low dose streptozotocin (STZ, 35 mg/kg)-induced T2D and HFF only, nondiabetic (controls-no STZ) rats were treated with the SSTR2 antagonists ZT-01/PRL-2903 or vehicle (n = 9-11/group) 60 min before an insulin tolerance test (ITT; 2-12 U/kg insulin aspart) or an oral glucose tolerance test (OGTT; 2 g/kg glucose via oral gavage) on separate days. Results: This rodent model of T2D is characterized by higher baseline glucose and HbA1c levels relative to HFF controls. T2D rats also had lower c-peptide levels at baseline and a blunted glucagon counterregulatory response to hypoglycemia when subjected to the ITT. SSTR2 antagonists increased the glucagon response and reduced incidence of hypoglycemia, which was more pronounced with ZT-01 than PRL-2903. ZT-01 treatment in the T2D rats increased glucagon levels above the control response within 60 min of dosing, and values remained elevated during the ITT (glucagon Cmax: 156 ± 50 vs. 77 ± 46 pg/mL, p < 0.01). Hypoglycemia incidence was attenuated with ZT-01 vs. controls (63% vs. 100%) and average time to hypoglycemia onset was also delayed (103.1 ± 24.6 vs. 66.1 ± 23.6 min, p < 0.05). ZT-01 administration at the OGTT onset increased the glucagon response without exacerbating hyperglycemia (2877 ± 806 vs. 2982 ± 781), potentially due to the corresponding increase in c-peptide levels (6251 ± 5463 vs. 14008 ± 5495, p = 0.013). Conclusion: Treatment with SSTR2 antagonists increases glucagon responses in a rat model of T2D and results in less hypoglycemia exposure. Future studies are required to determine the best dosing periods for chronic SSTR2 antagonism treatment in T2D.

Keywords: counterregulation; glucagon; hypoglycemia; somatostatin receptor antagonist; type 2 diabetes.

Grants and funding

The author(s) declare financial support was received for the research, authorship, and/or publication of this article. This work is supported by GlycoNet, a Government of Canada Networks of Centres of Excellence program (Grant # CD-85), by the Natural Sciences and Engineering Research Council of Canada (NSERC, Grant # 261306) and Zucara Therapeutics in grants and/or contracts to MCR PhD. NCD is supported with a Mitacs Accelerate Fellowship/Internship jointly funded by Mitacs Canada and Zucara Therapeutics.