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184 Insulin Sensitivity and Glucose Metabolism of Olanzapine and Combination Olanzapine and Samidorphan: A Phase 1 Exploratory Study in Healthy Volunteers

Published online by Cambridge University Press:  24 April 2020

William Martin
Affiliation:
Senior Director, Clinical Operations, Alkermes, Inc., Waltham, MA
Christine Graham
Affiliation:
Associate Medical Director, Clinical Research, Alkermes, Inc., Waltham, MA
Linda Morrow
Affiliation:
Chief Medical Officer, ProSciento, Inc., Chula Vista CA
Carine Beysen
Affiliation:
Senior Director, Clinical Research Innovation Services, ProSciento, Inc., Chula Vista, CA
Frederico G.S. Toledo
Affiliation:
Associate Professor of Medicine, University of Pittsburgh, Pittsburgh, PA
Daiva Bajorunas
Affiliation:
Chief Scientific and Medical Officer, Vault Bioventures, San Diego, CA
Ying Jiang
Affiliation:
Director, Biostatistics, Alkermes, Inc., Waltham, MA
Bernard Silverman
Affiliation:
Vice President, Clinical Strategy, Alkermes, Inc., Waltham, MA
David McDonnell
Affiliation:
Executive Medical Director, Clinical Science, Alkermes Pharma Ireland Limited, Dublin, Ireland
Mark N. Namchuk
Affiliation:
Senior Vice President, Research, Alkermes, Inc., Waltham, MA
John W. Newcomer
Affiliation:
President and Chief Executive Officer, Thriving Mind South Florida, Miami, FL
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Abstract:

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Background:

A combination of olanzapine and samidorphan (OLZ/SAM) is in development for schizophrenia to provide the efficacy of olanzapine while mitigating olanzapine-associated weight gain. The objective of this phase 1 exploratory study was to assess metabolic treatment effects of OLZ/SAM.

Methods:

Healthy, non-obese adults (18–40 years) were randomized 2:2:1 to once-daily OLZ/SAM, olanzapine, or placebo for 21 days. Assessments included oral glucose tolerance test (OGTT), hyperinsulinemic-euglycemic clamp, weight gain, and adverse event (AE) monitoring. Treatment effects were estimated with analysis of covariance.

Results:

Sixty subjects were randomized (OLZ/SAM, n=24; olanzapine, n=24; placebo, n=12); 19 (79.2%), 22 (91.7%), and 11 (91.7%), respectively, completed the study. In the OGTT, olanzapine led to significant hyperinsulinemia (P<0.0001) and significantly reduced insulin sensitivity (2-hour Matsuda index) at day 19 vs baseline (P=0.0012), changes not observed with OLZ/SAM. No significant between-group differences were observed for change from baseline in clamp-derived insulin sensitivity index at day 21. Least squares mean weight change from baseline was similar with OLZ/SAM (3.16 kg) and olanzapine (2.87 kg); both were significantly higher than placebo (0.57 kg; both P<0.01). Caloric intake significantly decreased from baseline to day 22 with OLZ/SAM (P=0.015) but not with olanzapine or placebo. Forty-nine subjects (81.7%) experienced ≥1 AE (OLZ/SAM, 87.5%; olanzapine, 79.2%; placebo, 75.0%).

Conclusions:

In this exploratory study, hyperinsulinemia and decreased insulin sensitivity were observed in the OGTT with olanzapine but not with OLZ/SAM or placebo. Clamp-derived insulin sensitivity index and weight changes were similar with OLZ/SAM and olanzapine in healthy subjects during the 3-week study.

Funding Acknowledgements:

This study was funded by Alkermes, Inc.

Type
Abstracts
Copyright
© Cambridge University Press 2020