schizophrenia psychosis
Schizophrenia trials have been revitalized by the approval of muscarinic receptor agonists (xanomeline-trospium/KarXT) β€” the first non-dopaminergic antipsychotic approved in decades β€” validating a long-hypothesized cholinergic mechanism and opening new mechanistic territory. Negative symptom treatment and cognitive impairment associated with schizophrenia (CIAS) remain critical unmet needs with no approved therapies.
Active trials investigate M1/M4 muscarinic agonists, trace amine-associated receptor 1 (TAAR1) agonists (ulotaront), glycine transporter inhibitors, cognitive remediation combined with pharmacotherapy, and long-acting injectable formulations to improve adherence. PANSS total score and negative symptom subscales are standard primary endpoints.
Disease Burden & Epidemiology
Schizophrenia affects approximately 24 million people globally — roughly 1 in 300 of the world population — according to the World Health Organization. In the United States, approximately 2.8 million adults (1.1% of the adult population) have a schizophrenia spectrum diagnosis. The condition typically emerges in late adolescence or early adulthood, with peak onset between ages 16 and 30; onset before puberty and after 45 is less common. Men tend to develop schizophrenia approximately 5 years earlier than women, with a slightly more severe course. Schizophrenia is associated with profound functional impairment: approximately 70–80% of patients have significant difficulties with employment, independent living, and social relationships. Life expectancy is reduced by 15–20 years compared to the general population, primarily due to cardiovascular disease, metabolic effects of antipsychotic medications, higher rates of smoking, and suicide (which accounts for approximately 5% of deaths). Despite availability of multiple antipsychotic medications, approximately 30% of patients have treatment-resistant schizophrenia (TRS) — inadequate response to two or more antipsychotics — for whom clozapine is the standard of care, though it carries significant monitoring requirements due to agranulocytosis risk. The economic cost of schizophrenia in the US exceeds $280 billion annually including direct and indirect costs.
Key Research Trends & Landmark Studies
The EMERGENT-2 and EMERGENT-3 Phase 3 trials of xanomeline-trospium (Cobenfy/KarXT) demonstrated a 9.6-point reduction in PANSS total score versus placebo — without the weight gain, metabolic effects, and extrapyramidal side effects characteristic of dopamine-blocking antipsychotics — leading to FDA approval in September 2024 as the first new antipsychotic mechanism in over 35 years. The GRANITE trial for ulotaront (TAAR1 agonist, Sunovion) showed positive Phase 2 results, though Phase 3 results were mixed, highlighting the challenges of mechanism translation. Long-acting injectable (LAI) trials have established that LAI formulations (paliperidone palmitate, aripiprazole monohydrate) reduce relapse rates by 30–50% versus oral medications in pragmatic effectiveness studies. For treatment-resistant schizophrenia, the CITOMED trial is evaluating augmentation strategies for clozapine non-responders. Digital biomarker trials using passive smartphone data — voice, movement, social interaction patterns — to predict psychotic relapse represent a growing research priority.
Patient Guide: How to Find & Join a Trial
People with schizophrenia spectrum disorders — including schizoaffective disorder — can participate in clinical trials at various stages of illness, from first-episode psychosis through chronic treatment-resistant disease. Psychiatric diagnosis must be confirmed using structured diagnostic criteria (DSM-5), typically administered by a psychiatrist or research clinician as part of the screening process. For acute treatment trials, a minimum severity threshold (typically PANSS total score ≥70–80) is required at baseline. For long-term effectiveness and relapse prevention trials, stable patients on current antipsychotic therapy may enroll without a required washout period. Patients with treatment-resistant schizophrenia (failed two or more adequate antipsychotic courses including one trial of clozapine in some studies) may be eligible for trials of novel mechanisms specifically designed for TRS. Academic psychiatry departments, community mental health centers affiliated with university research programs, and VA medical centers with mental health research divisions are the primary trial sites. Family members and caregivers often serve as study partners and may assist in consent and follow-up visit participation.