Proof of Mechanism and Target Engagement of Glutamatergic Drugs for the Treatment of Schizophrenia: RCTs of Pomaglumetad and TS-134 on Ketamine-induced Psychotic Symptoms and PharmacoBOLD in Healthy Volunteers

Overview

Journal Neuropsychopharmacology

Date 2020 May 14

PMID 32403118

Citations 25

Authors

Joshua T Kantrowitz

Jack Grinband

Donald C Goff

Adrienne C Lahti

Stephen R Marder

Lawrence S Kegeles

Ragy R Girgis

Tarek Sobeih

Melanie M Wall

Tse-Hwei Choo

Michael F Green

Yvonne S Yang

Junghee Lee

Guillermo Horga

John H Krystal

William Z Potter

Daniel C Javitt

Jeffrey A Lieberman

Affiliations

Soon will be listed here.

Abstract

Glutamate neurotransmission is a prioritized target for antipsychotic drug development. Two metabotropic glutamate receptor 2/3 (mGluR2/3) agonists (pomaglumetad [POMA] and TS-134) were assessed in two Phase Ib proof of mechanism studies of comparable designs and using identical clinical assessments and pharmacoBOLD methodology. POMA was examined in a randomized controlled trial under double-blind conditions for 10-days at doses of 80 or 320 mg/d POMA versus placebo (1:1:1 ratio). The TS-134 trial was a randomized, single-blind, 6-day study of 20 or 60 mg/d TS-134 versus placebo (5:5:2 ratio). Primary outcomes were ketamine-induced changes in pharmacoBOLD in the dorsal anterior cingulate cortex (dACC) and symptoms reflected on the Brief Psychiatric Rating Scale (BPRS). Both trials were conducted contemporaneously. 95 healthy volunteers were randomized to POMA and 63 to TS-134. High-dose POMA significantly reduced ketamine-induced BPRS total symptoms within and between-groups (p < 0.01, d = -0.41; p = 0.04, d = -0.44, respectively), but neither POMA dose significantly suppressed ketamine-induced dACC pharmacoBOLD. In contrast, low-dose TS-134 led to moderate to large within and between group reductions in both BPRS positive symptoms (p = 0.02, d = -0.36; p = 0.008, d = -0.82, respectively) and dACC pharmacoBOLD (p = 0.004, d = -0.56; p = 0.079, d = -0.50, respectively) using pooled across-study placebo data. High-dose POMA exerted significant effects on clinical symptoms, but not on target engagement, suggesting a higher dose may yet be needed, while the low dose of TS-134 showed evidence of symptom reduction and target engagement. These results support further investigation of mGluR2/3 and other glutamate-targeted treatments for schizophrenia.

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