The Impact of Xanomeline and Trospium Chloride on Cognitive Impairment in Acute Schizophrenia: Replication in Pooled Data From Two Phase 3 Trials

William P Horan; Colin Sauder; Philip D Harvey; Ian S Ramsay; Samantha E Yohn; Richard S E Keefe; Vicki G Davis; Steven M Paul; Stephen K Brannan

doi:10.1176/appi.ajp.20240076

The Impact of Xanomeline and Trospium Chloride on Cognitive Impairment in Acute Schizophrenia: Replication in Pooled Data From Two Phase 3 Trials

Am J Psychiatry. 2025 Mar 1;182(3):297-306. doi: 10.1176/appi.ajp.20240076. Epub 2024 Dec 11.

Authors

William P Horan¹, Colin Sauder¹, Philip D Harvey¹, Ian S Ramsay¹, Samantha E Yohn¹, Richard S E Keefe¹, Vicki G Davis¹, Steven M Paul¹, Stephen K Brannan¹

Affiliation

¹ Bristol Myers Squibb, Boston (Horan, Sauder, Ramsay, Yohn, Paul, Brannan); University of Miami Miller School of Medicine, Miami (Harvey); Duke University School of Medicine, Durham (Keefe); Statistical Consultant, Chapel Hill (Davis).

PMID: 39659157
DOI: 10.1176/appi.ajp.20240076

Abstract

Objective: Xanomeline and trospium chloride (formerly known as KarXT), a novel M₁/M₄ muscarinic receptor agonist, demonstrated efficacy across phase 2 and 3 trials as monotherapy for the treatment of inpatients with acute schizophrenia on the Positive and Negative Syndrome Scale total score primary endpoint. In the phase 2 trial, xanomeline/trospium improved performance on a cognitive outcome measure in the subgroup of participants with clinically significant baseline cognitive impairment. The authors sought to confirm this finding using data from two phase 3 trials.

Methods: Data were pooled from two 5-week inpatient trials of xanomeline/trospium monotherapy in patients with acute schizophrenia. The statistical analysis plan prespecified comparisons of cognitive composite score changes between xanomeline/trospium and placebo in the full sample and the cognitively impaired (≤1 SD below norms at baseline) subgroup.

Results: There was no significant xanomeline/trospium effect in the full sample (N=357); however, in the impaired subgroup, xanomeline/trospium (N=71) had a significantly greater benefit for cognition compared with placebo (N=66; least squares mean difference=0.31, SE=0.10; d=0.54). The xanomeline/trospium effect size increased significantly with a more stringent baseline impairment threshold (≤-1.5 SD; d=0.80). Improvements in cognition were minimally correlated with concurrent changes in total, positive, and negative symptoms in both treatment groups.

Conclusions: Participants with acute schizophrenia with prespecified impairments demonstrated significant cognitive improvement with xanomeline/trospium compared with placebo. This result directly confirms earlier findings. This benefit is not attributable to changes in symptoms, despite substantial evidence of efficacy for psychosis. Evaluation of xanomeline/trospium's potential for cognitive enhancement in a well-controlled trial of stable patients with cognitive impairment is warranted.

Keywords: Cognition/Learning/Memory; Schizophrenia Spectrum and Other Psychotic Disorders.

Publication types

Clinical Trial, Phase II
Clinical Trial, Phase III
Randomized Controlled Trial

MeSH terms

Acute Disease
Adult
Antipsychotic Agents / therapeutic use
Benzilates* / therapeutic use
Cognitive Dysfunction* / drug therapy
Double-Blind Method
Female
Humans
Male
Middle Aged
Nortropanes* / therapeutic use
Pyridines
Schizophrenia* / complications
Schizophrenia* / drug therapy
Thiadiazoles
Treatment Outcome

Substances

Antipsychotic Agents
Benzilates
Nortropanes
trospium chloride
xanomeline
Pyridines
Thiadiazoles