An open-label study on ulotaront's effects on insulin-glucose regulation in schizophrenia patients with metabolic syndrome and prediabetes: Part I.
Snezana Milanovic, Robert Lew, Kuangnan Xiong, Emily Casavant, Gerard Galluppi, Yu-Luan Chen, Yongquan Lai, Manu Chakravarthy, Clay Dehn, Kenneth Koblan, Seth C Hopkins
Abstract
Open AccessAIMS: Ulotaront is an investigational trace amine-associated receptor 1 (TAAR1) agonist demonstrated to slow gastric emptying in schizophrenia patients with metabolic syndrome (MetSyn) and prediabetes type 2. Here we evaluate the effects of ulotaront on glucose-insulin dynamics in schizophrenia patients with MetSyn and prediabetes. METHODS AND METHODS: NCT05463770 was a Phase 1b clinical trial, with an open-label, multi-dose design comparing ulotaront's metabolic effects to each participant's baseline of prior antipsychotic treatment. Oral glucose tolerance test (oGTT), a mixed meal tolerance test (MMTT) and a spirulina breath test (GEBT) were conducted at a baseline of prior antipsychotic medication and repeated after up to 3 weeks of twice-a-day dosing of ulotaront. RESULTS: In oGTT and MMTT, mean changes from baseline AUCs for glucose, c-peptide and insulin were -19.7 h×mg/dL, -269 h×pg/mL, -41.0 h×uIU/mL, and -10.8 h×mg/dL, -2860 h×pg/mL, -132 h×mg/dL, respectively. Insulin response during the MMTT reached nominal statistical significance (p = 0.021, effect size = -0.7). The mean change from baseline gastric emptying time was -0.60 min. CONCLUSIONS: Despite limited sample size, primary endpoints favoured ulotaront over prior antipsychotics with respect to a reduction trend in glucose, c-peptide and insulin. The insulin response after a solid meal was nominally significant, suggesting that semi-chronic twice-a-day dosing of ulotaront might improve insulin dynamics in schizophrenia patients at high diabetes risk.