NCT01292577
- Objective
- Not yet disclosed
- Design
- Not yet disclosed
- Participants
- Not yet disclosed
- Primary endpoint
- Not yet disclosed
- Results
- Results not yet reported in public domain
pharma · Cocaine-Related Disorders · Cocaine Dependence · DRUG
BRIGHT MINDS BIOSCIENCES INC.
Bright Minds Biosciences is a pharma organization headquartered in New York, USA. It trades on NYSE under ticker DRUG. Primary therapeutic focus areas include Cocaine-Related Disorders, Cocaine Dependence, Nicotine Depen
Phase 2 · other · Schizophrenia
CET/PT (internal code 118404) is a Phase 2 program developed by Bright Minds Biosciences Inc. for the treatment of schizophrenia. The program's mechanism of action and specific molecular target have not been disclosed. As of April 2020, the program had completed Phase 2 development, representing the most recent disclos
Internal code 118404
CET/PT (internal code 118404) is a Phase 2 program developed by Bright Minds Biosciences Inc. for the treatment of schizophrenia. The program's mechanism of action and specific molecular target have not been disclosed. As of April 2020, the program had completed Phase 2 development, representing the most recent disclosed milestone. The modality is classified as 'other,' indicating it does not fit standard small-molecule or biologic categories. Bright Minds Biosciences has not disclosed partnership arrangements, licensing terms, or regulatory interactions for this candidate. The competitive landscape for schizophrenia treatment includes multiple approved agents spanning antipsychotics (aripiprazole, paliperidone ER, iloperidone) and adjunctive therapies (valbenazine, vortioxetine, minocycline). Peak sales projections, consensus analyst positioning, and next-milestone timelines remain undisclosed. The program's current development status beyond the April 2020 completion milestone is not yet reported.
Schizophrenia affects millions globally and represents a significant unmet medical need despite the availability of multiple antipsychotic agents. Approximately 30–40% of patients with schizophrenia exhibit treatment resistance or inadequate response to standard therapies, and side-effect burdens—including metabolic, motor, and cognitive effects—drive the need for novel mechanisms. The competitive landscape includes established agents (clozapine, aripiprazole, paliperidone ER) and newer adjunctive options (valbenazine for tardive dyskinesia, vortioxetine for cognitive symptoms), yet clinical heterogeneity and individual variability in treatment response sustain demand for differentiated approaches.
Bright Minds Biosciences' positioning in this market includes multiple programs across schizophrenia and related indications. The CET/PT program's undisclosed mechanism and modality suggest potential differentiation from conventional dopamine antagonists or serotonergic agents. Completion of Phase 2 as of April 2020 indicates the program has generated preliminary efficacy and safety data, though specific endpoints, patient populations studied, and comparative positioning versus existing therapies remain proprietary. Commercial significance depends on efficacy profile, tolerability advantages, and regulatory pathway clarity—factors not yet disclosed in public records.
Modality: Other (not classified as small-molecule or biologic)
Indication: Schizophrenia
Mechanism of Action: Not yet disclosed
Target: Not yet disclosed
Route of Administration: Not yet disclosed
Molecular Type: Modality classified as 'other'
Also known as: schizophrenia 12, schizophrenia (disease), SCZD
A major psychotic disorder characterized by abnormalities in the perception or expression of reality. It affects the cognitive and psychomotor functions. Common clinical signs and symptoms include delusions, hallucinations, disorganized thinking, and retreat from reality.
ClinicalTrials.gov lists 2,921 registered studies for Schizophrenia (AACT aggregate).
Phase breakdown: NA (1,441), PHASE4 (414), PHASE3 (377), PHASE2 (297), PHASE1 (276), PHASE1/PHASE2 (52), PHASE2/PHASE3 (42), EARLY_PHASE1 (22)
Common investigational therapies:
Disease data sourced from MONDO Disease Ontology (MONDO:0005090), Orphanet — schizophrenia, NCT00000371, NCT00000372, NCT00000374, NCT00000387, NCT00001192, AACT (ClinicalTrials.gov aggregate), ClinicalTrials.gov, Open Targets Platform (CC BY 4.0).
Phase 2 Completion
CET/PT Phase 2 program completed; specific endpoints, patient outcomes, and next-stage plans not yet disclosed.
The schizophrenia treatment market includes multiple approved antipsychotics and adjunctive agents. Clozapine, developed by Bright Minds Biosciences, remains a gold-standard atypical antipsychotic for treatment-resistant schizophrenia despite side-effect constraints. Aripiprazole (Otsuka Beijing Research Institute), paliperidone ER (Hospital Authority, Hong Kong), and iloperidone (Vanda Pharmaceuticals) represent conventional dopamine-modulating approaches. Newer agents address specific symptom domains: valbenazine (Neurocrine Biosciences) targets tardive dyskinesia, vortioxetine (Takeda) addresses cognitive and depressive symptoms, and minocycline (Bright Minds Biosciences) serves as an adjunctive anti-inflammatory augmentation strategy. Ramelteon (Takeda) and dexmedetomidine (BioXcel Therapeutics) address sleep and agitation. Perseris (Indivior) and Intensify SZ (Disc Medicine) represent formulation and combination innovations. CET/PT's competitive positioning remains unclear pending disclosure of mechanism, efficacy data, and differentiation strategy.
| Therapy | Company | Mechanism | Status |
|---|---|---|---|
| Clozapine | BRIGHT MINDS BIOSCIENCES INC. | small_molecule | approved |
| Iloperidone | Vanda Pharmaceuticals Netherlands B.V. | small_molecule | approved |
| Ramelteon | Takeda | small_molecule | approved |
| PERSERIS | Indivior Pty Ltd | small_molecule | approved |
| INTENSIFY SZ | Disc Medicine | small_molecule | approved |
| Varenicline | BRIGHT MINDS BIOSCIENCES INC. | small_molecule | approved |
| Aripiprazole | Otsuka Beijing Research Institute | small_molecule | approved |
| Paliperidone ER | Hospital Authority, Hong Kong | small_molecule | approved |
| Vortioxetine | Takeda | small_molecule | approved |
| Valbenazine | NEUROCRINE BIOSCIENCES INC | small_molecule | approved |
| Minocycline | BRIGHT MINDS BIOSCIENCES INC. | small_molecule | approved |
| Dexmedetomidine | BioXcel Therapeutics | small_molecule | approved |
| ZIPRASIDONE HYDROCHLORIDE | — | Dopamine D2 receptor antagonist | Approved |
| TRIFLUOPERAZINE HYDROCHLORIDE | — | D2-like dopamine receptor antagonist | Approved |
| THIOTHIXENE | — | Dopamine D2 receptor antagonist | Approved |
| SAMIDORPHAN L-MALATE | — | Delta opioid receptor partial agonist | Approved |
| RISPERIDONE | — | Serotonin 2a (5-HT2a) receptor antagonist | Approved |
| QUETIAPINE FUMARATE | — | Serotonin 2c (5-HT2c) receptor antagonist | Approved |
| PROCHLORPERAZINE | — | Dopamine D2 receptor antagonist | Approved |
| PERPHENAZINE | — | Dopamine D2 receptor antagonist | Approved |
Additional associated therapies sourced from Open Targets Platform (CC0), linked to NovaPharmaNews drug profiles where matched.
FDA Status: Not yet disclosed
EMA Status: Not yet disclosed
PMDA (Japan) Status: Not yet disclosed
NMPA (China) Status: Not yet disclosed
CET/PT completed Phase 2 development as of April 13, 2020. No regulatory submissions, approvals, or interactions with major regulatory agencies have been disclosed. The program's regulatory pathway, anticipated filing strategy, and timeline to potential regulatory review remain proprietary.
CET/PT is a Phase 2 program in development by Bright Minds Biosciences Inc. for the treatment of schizophrenia.
No. CET/PT is in Phase 2 development and has not been approved by the FDA or other major regulatory agencies.
The mechanism of action for CET/PT has not been disclosed by the sponsor.
Bright Minds Biosciences Inc. is the sponsor and developer of CET/PT.
CET/PT is classified as 'other' modality, meaning it does not fit standard small-molecule or biologic categories; specific details are not yet disclosed.
NCT01292577 is the identified trial associated with CET/PT; detailed trial design, results, and outcomes have not been publicly reported.
CET/PT completed Phase 2 development on April 13, 2020, according to the latest disclosed milestone.
The internal code for CET/PT is 118404.
No partnership or licensing arrangement has been disclosed for CET/PT.
The specific molecular target for CET/PT has not been disclosed.
Clozapine is an approved atypical antipsychotic also associated with Bright Minds Biosciences; CET/PT's mechanism and comparative efficacy remain undisclosed.
Approved competitors include aripiprazole, paliperidone ER, iloperidone, valbenazine, vortioxetine, minocycline, and other antipsychotics and adjunctive agents.
The route of administration for CET/PT has not been disclosed.
Peak sales projections for CET/PT have not been disclosed.
CET/PT completed Phase 2 as of April 2020; the current status and next-milestone timeline have not been disclosed.
Consensus analyst positioning on CET/PT has not been disclosed.
CET/PT → Drug → Target → Indication → Company → Trials → Competitors
Strategic Implications: Bright Minds Biosciences' CET/PT program represents a Phase 2-stage asset in a mature but therapeutically active indication. The April 2020 completion milestone suggests the sponsor has generated preliminary efficacy and safety signals sufficient to advance; however, the absence of disclosed data, mechanism, or next-milestone timeline limits visibility into commercial probability and competitive positioning.
Competitive Implications: The schizophrenia market remains fragmented across conventional antipsychotics, atypical agents, and symptom-specific adjunctive therapies. CET/PT's undisclosed modality and mechanism create uncertainty regarding its niche—whether it targets treatment resistance, cognitive symptoms, tolerability, or a novel pathway. Differentiation from clozapine, aripiprazole, and valbenazine will be critical to market entry success.
Future Catalysts: Publication of Phase 2 efficacy and safety data; disclosure of mechanism of action and target; announcement of Phase 3 initiation or regulatory pathway; partnership or licensing announcements; comparative efficacy or tolerability claims versus standard-of-care agents.
Expected Milestones: Timing of Phase 3 initiation, regulatory pre-submission meetings, and potential filing dates remain undisclosed and dependent on Phase 2 outcomes and sponsor strategy.
Concise, citable answers optimized for AI answer engines.
Intelligence compiled from public regulatory and clinical sources (FDA, EMA, ClinicalTrials.gov and company disclosures). Figures may be editorial or analyst estimates; verify against primary sources before relying on them.