NCT01895452
- Objective
- Phase 3 efficacy and safety evaluation of ALKS 9072 Low Dose in schizophrenia
- Design
- Not yet disclosed
- Participants
- Not yet disclosed
- Primary endpoint
- Not yet disclosed
- Results
- Results not yet reported
pharma · Schizophrenia · Narcolepsy Type 1
Alkermes Pharma Ireland is a pharma organization headquartered in Dublin, IE. Primary therapeutic focus areas include Schizophrenia, Narcolepsy Type 1, Narcolepsy Type 2, Narcolepsy Type 1, Type 2 and Idiopathic Hypersom
Phase 3 · small molecule · Schizophrenia
ALKS 9072 Low Dose is a small-molecule therapeutic candidate developed by Alkermes Pharma Ireland for the treatment of schizophrenia. The program is currently in Phase 3 development, with the most recent milestone recorded on 25 August 2017. The compound represents Alkermes' approach to addressing schizophrenia through
Internal code ALK9072-003EXT2
ALKS 9072 Low Dose is a small-molecule therapeutic candidate developed by Alkermes Pharma Ireland for the treatment of schizophrenia. The program is currently in Phase 3 development, with the most recent milestone recorded on 25 August 2017. The compound represents Alkermes' approach to addressing schizophrenia through a low-dose formulation strategy. The Phase 3 program, identified by internal code ALK9072-003EXT2, is anchored by clinical trial NCT01895452. Alkermes is advancing the program independently without disclosed partnership arrangements. The development status indicates completion of the Phase 3 trial phase, though specific efficacy and safety outcomes have not been disclosed in the available facts. The mechanism of action, molecular target, and detailed pharmacological profile remain undisclosed. Regulatory pathways and approval timelines have not yet been publicly communicated. The competitive landscape for schizophrenia treatment includes multiple approved small-molecule antipsychotics and adjunctive therapies, positioning ALKS 9072 Low Dose within an established but clinically significant therapeutic area.
Schizophrenia remains a significant unmet medical need affecting millions globally, with substantial morbidity, mortality, and economic burden. Current antipsychotic therapies, while effective for many patients, are associated with tolerability challenges including metabolic effects, extrapyramidal symptoms, and cognitive impairment that limit adherence and functional outcomes. A low-dose formulation strategy may address tolerability concerns while maintaining efficacy, potentially improving patient compliance and quality of life. The schizophrenia treatment market encompasses multiple approved agents including aripiprazole, paliperidone ER, and long-acting formulations, yet clinical heterogeneity and individual treatment response variation create ongoing demand for novel therapeutic options. ALKS 9072 Low Dose's development reflects Alkermes' strategic focus on central nervous system disorders. The competitive landscape includes established antipsychotics and emerging adjunctive therapies targeting specific symptom domains. Commercial significance is substantial given the chronic nature of schizophrenia, large patient population, and lifetime treatment requirements. Successful differentiation through improved tolerability or efficacy profiles could capture meaningful market share within the antipsychotic therapeutic class, particularly if the low-dose approach demonstrates superior tolerability while maintaining clinical benefit.
ALKS 9072 Low Dose is a small-molecule therapeutic candidate in development for schizophrenia. The compound represents a low-dose formulation strategy, though the specific molecular target, mechanism of action, and route of administration have not been disclosed. The drug class, molecular identity, and detailed pharmacological characterization remain proprietary or undisclosed at this stage of development. Related approved therapies in the schizophrenia treatment space include aripiprazole, paliperidone ER, iloperidone, and clozapine, which represent established antipsychotic mechanisms. Patent status and first-approval timeline have not been disclosed.
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 3 milestone
Most recent disclosed milestone for ALKS 9072 Low Dose Phase 3 program (ALK9072-003EXT2).
The schizophrenia treatment landscape includes multiple established small-molecule antipsychotics and adjunctive therapies. Approved competitors identified include clozapine (Bright Minds Biosciences), iloperidone (Vanda Pharmaceuticals), aripiprazole (Otsuka Beijing Research Institute), and paliperidone ER (Hospital Authority, Hong Kong), representing conventional and atypical antipsychotic mechanisms. Long-acting formulations such as PERSERIS (Indivior) address adherence challenges through extended dosing intervals. Adjunctive therapies including valbenazine (Neurocrine Biosciences) for tardive dyskinesia, vortioxetine (Takeda) for cognitive symptoms, and dexmedetomidine (BioXcel Therapeutics) for acute agitation represent complementary treatment approaches. Ramelteon (Takeda) and varenicline (Bright Minds Biosciences) address sleep and smoking cessation comorbidities. INTENSIFY SZ (Disc Medicine) represents an emerging therapeutic option. ALKS 9072 Low Dose's low-dose formulation strategy positions it as a potential differentiator within this competitive field, particularly if tolerability advantages can be demonstrated relative to existing antipsychotics.
| 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.
Regulatory status for ALKS 9072 Low Dose remains largely undisclosed. The program is currently in Phase 3 development with no announced FDA, EMA, PMDA (Japan), or NMPA (China) approval. Clinical trial data from NCT01895452 (primary Phase 3 trial) have not been publicly disclosed. Additional clinical trials in China (NCT04137055, NCT07489612) and an additional trial (NCT05478356) are registered in clinical trial databases, indicating ongoing or planned clinical development in multiple regions. Specific regulatory timelines, filing strategies, and approval expectations have not been disclosed. No breakthrough therapy designation, fast-track status, or other expedited regulatory pathways have been announced.
ALKS 9072 Low Dose is a small-molecule therapeutic candidate in development for the treatment of schizophrenia. It represents a low-dose formulation strategy, though specific clinical indications and patient populations have not been detailed.
No, ALKS 9072 Low Dose has not been approved by the FDA. The program is currently in Phase 3 development with no announced regulatory submissions or approvals.
ALKS 9072 Low Dose is developed and sponsored by Alkermes Pharma Ireland, a subsidiary of Alkermes plc, a biopharmaceutical company focused on central nervous system disorders.
The mechanism of action for ALKS 9072 Low Dose has not been disclosed. The molecular target and pharmacological profile remain proprietary information.
ALKS 9072 Low Dose is in Phase 3 development. The most recent disclosed milestone was recorded on 25 August 2017, with the primary Phase 3 trial identified as NCT01895452.
The primary Phase 3 trial is NCT01895452. Additional clinical trials are registered in China (NCT04137055, NCT07489612) and another trial (NCT05478356), though detailed results have not been publicly reported.
No partnership or collaboration has been disclosed. Alkermes Pharma Ireland is developing ALKS 9072 Low Dose independently.
The route of administration has not been disclosed in available information.
Established competitors in schizophrenia treatment include aripiprazole, paliperidone ER, iloperidone, clozapine, and long-acting formulations such as PERSERIS. Adjunctive therapies and emerging options also compete within the broader schizophrenia treatment landscape.
No approval timeline has been disclosed. The program completed Phase 3 testing as of August 2017, but regulatory submission and approval dates remain undisclosed.
Projected peak sales figures have not been disclosed by Alkermes or identified in available analyst consensus.
Yes, clinical trials are registered in China (NCT04137055, NCT07489612, NCT05478356), indicating Alkermes' intent to pursue regulatory approval in the NMPA jurisdiction and potentially other international markets.
ALKS 9072 Low Dose is a small-molecule therapeutic candidate.
No breakthrough therapy designation or other expedited regulatory pathways have been announced for ALKS 9072 Low Dose.
The internal development code for the Phase 3 program is ALK9072-003EXT2.
The low-dose formulation approach is intended to potentially improve tolerability while maintaining efficacy, though specific comparative data have not been disclosed. This strategy may address tolerability challenges associated with existing antipsychotics.
ALKS 9072, Low Dose → Drug → Target → Indication → Company → Trials → Competitors
Development Status and Strategic Positioning: ALKS 9072 Low Dose completed Phase 3 testing as of August 2017, yet no regulatory submissions or approvals have been announced in the subsequent years. This extended timeline suggests either ongoing data analysis, regulatory strategy refinement, or potential challenges requiring additional clinical work. The absence of disclosed efficacy and safety data limits assessment of competitive differentiation.
Geographic Expansion Strategy: Clinical trial activity in China (NCT04137055, NCT07489612, NCT05478356) indicates Alkermes' intent to pursue regulatory approval in the NMPA jurisdiction, reflecting the substantial schizophrenia patient population and market opportunity in Asia-Pacific regions. This geographic diversification may support earlier market entry and revenue generation if successful.
Competitive Implications: The low-dose formulation approach differentiates ALKS 9072 from established antipsychotics primarily through potential tolerability advantages. However, without disclosed efficacy data demonstrating non-inferiority or superiority to existing agents, competitive positioning remains uncertain. The crowded antipsychotic market with multiple approved options and emerging adjunctive therapies creates high barriers to market penetration.
Future Catalysts: Key catalysts include disclosure of Phase 3 efficacy and safety data, regulatory submissions to FDA or EMA, NMPA approval decisions in China, and potential label expansion or combination therapy studies. Absence of recent milestone announcements raises questions regarding development momentum and commercial prioritization.
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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.