NCT02357797
- Objective
- Not yet disclosed
- Design
- Not yet disclosed
- Participants
- Not yet disclosed
- Primary endpoint
- Not yet disclosed
- Results
- Results not yet reported
pharma · Diabetes Mellitus · Hemophilia A
Takeda is a pharma organization headquartered in Cambridge, USA. Primary therapeutic focus areas include Diabetes Mellitus, Hemophilia A, Crohn's Disease, Hypertension, Type 2 Diabetes Mellitus. NovaPharmaNews links 1179
Approved · small molecule · Schizophrenia
Vortioxetine (BRINTELLIX) is an oral small-molecule antidepressant developed by Takeda for schizophrenia treatment. The drug is classified within the nervous system therapeutic category (ATC N06) and has achieved approved regulatory status. Vortioxetine was originally developed by H. Lundbeck A/S and received European
Internal code 14-645
Vortioxetine (BRINTELLIX) is an oral small-molecule antidepressant developed by Takeda for schizophrenia treatment. The drug is classified within the nervous system therapeutic category (ATC N06) and has achieved approved regulatory status. Vortioxetine was originally developed by H. Lundbeck A/S and received European approval on 27 November 2025. In the United States, multiple generic manufacturers including Alkem Labs, Cipla, Macleods Pharmaceuticals, and Prinston Pharma hold approved applications (ANDA211024, ANDA211085, ANDA211089, ANDA211165), indicating mature market penetration. The program carries internal code 14-645 within Takeda's portfolio. The most recent disclosed milestone occurred on 8 February 2024, though specific milestone details remain undisclosed. The drug is administered orally and represents an established therapeutic option in the nervous system disorder space. Takeda's strategy appears focused on maintaining market presence through approved formulations rather than active clinical development, with the program classified as active status.
Schizophrenia represents a significant unmet medical need affecting millions globally, with substantial morbidity, mortality, and socioeconomic burden. Antidepressant therapies addressing comorbid depression in schizophrenia populations remain clinically relevant, as depressive symptoms frequently complicate schizophrenia management and worsen outcomes. Vortioxetine's oral administration and established safety profile position it within a competitive therapeutic landscape that includes multiple approved agents targeting neuropsychiatric conditions. The competitive set includes diverse mechanisms: duloxetine (serotonin-norepinephrine reuptake inhibitor), memantine (NMDA antagonist), donepezil (acetylcholinesterase inhibitor via Exelon), esketamine (SPRAVATO, NMDA antagonist), and emerging agents such as zurzuvae and lecanemab (LEQEMBI). The presence of multiple generic manufacturers in the US market indicates substantial commercial opportunity, though pricing pressure from generics limits peak revenue potential. Patient populations with schizophrenia-spectrum disorders and comorbid depressive symptoms represent the primary target demographic. Takeda's maintenance of active status suggests ongoing commercial relevance despite mature market positioning, with generic competition indicating established clinical acceptance and reimbursement pathways.
Drug Class: Antidepressant; Nervous System Agent (ATC N06)
Modality: Small-molecule oral formulation
Route of Administration: Oral
Brand Name: BRINTELLIX
International Nonproprietary Name (INN): Vortioxetine
Mechanism of Action: Not disclosed in available facts
Molecular Target: Not disclosed in available facts
Related Therapies: Serotonin-norepinephrine reuptake inhibitors (duloxetine), NMDA antagonists (memantine, esketamine), acetylcholinesterase inhibitors (donepezil), monoamine oxidase inhibitors (agomelatine/VALDOXAN)
First Approval: European approval 27 November 2025 by H. Lundbeck A/S; US generic approvals 2024 (exact dates not disclosed)
Patent Status: Not disclosed in available facts
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).
Latest milestone disclosed
Most recent program milestone reported; specific details not yet disclosed.
EMA approval
Vortioxetine (BRINTELLIX) approved by European Medicines Agency under H. Lundbeck A/S as marketing authorization holder.
Vortioxetine operates within a crowded neuropsychiatric therapeutic landscape. Direct antidepressant competitors include duloxetine (APO-DULOXETINE, Alphapharm), representing the serotonin-norepinephrine reuptake inhibitor class. Broader schizophrenia and depression management includes memantine (MEMANTINE MERZ, Amneal Pharma Europe), donepezil (EXELON, Novartis), and agomelatine (VALDOXAN). Emerging rapid-acting agents include esketamine (SPRAVATO, Janssen-Cilag) and zurzuvae, representing novel mechanisms in treatment-resistant depression. Cognitive and neurodegenerative support agents such as lecanemab (LEQEMBI) and idebenone (RAXONE) address related neurological pathology. Psychostimulants including solriamfetol (SUNOSI) target wakefulness in neuropsychiatric populations. The competitive set reflects heterogeneous mechanisms (monoamine reuptake inhibition, NMDA antagonism, acetylcholinesterase inhibition, AMPA potentiation), suggesting vortioxetine's positioning as an established oral option within a diversified treatment armamentarium. Generic availability through multiple US manufacturers (Alkem, Cipla, Macleods, Prinston Pharma) indicates mature market competition and pricing pressure, contrasting with branded premium-priced agents like SPRAVATO and emerging therapies.
| Therapy | Company | Mechanism | Status |
|---|---|---|---|
| TUZULBY | Amneal Pharma Europe Ltd | — | approved |
| APO-DULOXETINE | Alphapharm Pty Ltd | — | approved |
| MEMANTINE MERZ | Amneal Pharma Europe Ltd | — | approved |
| EXELON | Novartis Pharmaceuticals | — | approved |
| BLECTIFOR | Viridian Pharma Ltd | — | approved |
| ZURZUVAE | — | — | approved |
| PEYONA (PREVIOUSLY NYMUSA) | — | — | approved |
| VALDOXAN | — | — | approved |
| LEQEMBI | — | — | approved |
| RAXONE | — | — | approved |
| SPRAVATO | Janssen-Cilag Pty Ltd | — | approved |
| SUNOSI | — | — | 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.
European Union: Vortioxetine (BRINTELLIX) approved 27 November 2025 by the European Medicines Agency under marketing authorization holder H. Lundbeck A/S (EMEA/H/C/002717). Full EMA product information available at https://www.ema.europa.eu/en/medicines/human/EPAR/brintellix
United States: Multiple generic applications approved: ANDA211024 (Alkem Labs Ltd), ANDA211085 (Cipla Ltd), ANDA211089 (Macleods Pharmaceuticals Ltd), ANDA211165 (Prinston Pharma Inc). Approval dates not yet disclosed. FDA data accessible via https://open.fda.gov/apis/drug/drugsfda/
Japan (PMDA): Regulatory status not yet disclosed
China (NMPA): Regulatory status not yet disclosed
Loss of Exclusivity (LOE) Date: Not yet disclosed
Vortioxetine (BRINTELLIX) is indicated for schizophrenia treatment. It is an oral antidepressant classified in the nervous system therapeutic category (ATC N06).
Yes. Vortioxetine received European Medicines Agency approval on 27 November 2025 under H. Lundbeck A/S. Multiple generic formulations are approved in the United States through applications by Alkem Labs, Cipla, Macleods Pharmaceuticals, and Prinston Pharma.
The specific mechanism of action is not yet disclosed in available program documentation.
The molecular target is not yet disclosed in available program documentation.
Vortioxetine is administered orally as a small-molecule formulation.
H. Lundbeck A/S is the original developer and European marketing authorization holder. US generic manufacturers include Alkem Labs Ltd, Cipla Ltd, Macleods Pharmaceuticals Ltd, and Prinston Pharma Inc. Takeda holds the program within its portfolio.
NCT02357797 is disclosed as a trial associated with the program, though trial objectives, design, participant numbers, endpoints, and results are not yet disclosed.
The brand name is BRINTELLIX.
The internal program code is 14-645.
Vortioxetine is approved and active. The most recent milestone was disclosed on 8 February 2024, though specific details remain undisclosed.
Yes. Four US generic applications are approved: ANDA211024, ANDA211085, ANDA211089, and ANDA211165, indicating multiple generic manufacturers have market access.
Vortioxetine is classified as a nervous system agent (ATC N06), specifically an antidepressant used in neuropsychiatric conditions.
No partner or licensee is disclosed for Takeda's program, though H. Lundbeck A/S is the original developer and European marketing authorization holder.
The loss of exclusivity date is not yet disclosed.
Projected peak sales are not yet disclosed.
Competitors include duloxetine (APO-DULOXETINE), memantine (MEMANTINE MERZ), donepezil (EXELON), esketamine (SPRAVATO), agomelatine (VALDOXAN), and emerging agents such as zurzuvae and lecanemab (LEQEMBI).
Regulatory status in Japan (PMDA) and China (NMPA) is not yet disclosed.
Vortioxetine → Drug → Target → Indication → Company → Trials → Competitors
Strategic Positioning: Takeda maintains vortioxetine as an active approved program despite mature market status and generic competition, suggesting strategic value in established reimbursement pathways and clinical acceptance for schizophrenia-related depressive symptoms. The 8 February 2024 milestone, though undisclosed in detail, may indicate manufacturing, supply chain, or commercial optimization activities rather than clinical advancement.
Competitive Implications: Generic availability through four US manufacturers indicates commoditization and pricing pressure. Vortioxetine competes against both established agents (duloxetine, memantine) and emerging rapid-acting therapies (esketamine, zurzuvae). The lack of disclosed mechanism of action and molecular target limits differentiation messaging versus competitors with well-characterized pharmacology.
Clinical Development Status: No active clinical trials disclosed beyond NCT02357797, which lacks reported results. Absence of phase 3 or label expansion activities suggests Takeda is not pursuing additional indications or populations for schizophrenia treatment.
Future Catalysts: Potential catalysts include publication of NCT02357797 results, label expansion announcements, or manufacturing/supply announcements. No expected next milestone is currently disclosed. Regulatory actions in Japan (PMDA) or China (NMPA) could expand market access.
Commercial Outlook: Peak sales projections remain undisclosed. Generic competition limits revenue potential; market value derives from established clinical use and reimbursement infrastructure rather than patent protection or clinical novelty.
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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.