NCT01051531
- Objective
- Not yet disclosed
- Design
- Not yet disclosed
- Participants
- Not yet disclosed
- Primary endpoint
- Not yet disclosed
- Results
- Results not yet reported in available facts
pharma · Colitis, Ulcerative · Multiple Myeloma
Janssen Cilag International NV
Janssen-Cilag Farmaceutica Ltda is a pharma organization headquartered in São Paulo, EU. Primary therapeutic focus areas include Colitis, Ulcerative, Multiple Myeloma, Diabetes Mellitus, Type 2, Depressive Disorder, Majo
Phase 3 · small molecule · Schizophrenia
Paliperidone palmitate is a long-acting intramuscular antipsychotic developed by Janssen Cilag International NV for the treatment of schizophrenia. The active moiety, paliperidone, is a dopamine D2 receptor antagonist and serotonin 5-HT2a receptor antagonist belonging to the nervous system therapeutic class. The palmit
Internal code CR013612
Paliperidone palmitate is a long-acting intramuscular antipsychotic developed by Janssen Cilag International NV for the treatment of schizophrenia. The active moiety, paliperidone, is a dopamine D2 receptor antagonist and serotonin 5-HT2a receptor antagonist belonging to the nervous system therapeutic class. The palmitate ester formulation enables extended-release delivery via intramuscular injection, addressing medication adherence challenges in chronic schizophrenia management.
The program has completed Phase 3 clinical development as of October 2024. Paliperidone palmitate has achieved regulatory approval in multiple jurisdictions: the United States (NDA022264, NDA207946, NDA216352 approved; multiple generic ANDAs also approved), the European Union (EMEA/H/C/000746 and related product numbers authorized as of July 2024), and Australia (TGA-approved since 2008 with multiple PBS listings). The oral paliperidone formulation (INVEGA brand) has been approved since 2008 in Australia and carries multiple regulatory authorizations globally.
Janssen's strategy leverages the established efficacy and tolerability profile of paliperidone in the competitive antipsychotic market. The intramuscular depot formulation addresses a key clinical need for improved treatment adherence in schizophrenia patients. With Phase 3 completion and regulatory approvals already in place across major markets, the program represents a mature therapeutic option in the antipsychotic class, competing against multiple established agents including aripiprazole (ABILIFY), risperidone generics, and other dopamine antagonists.
Schizophrenia affects millions globally and remains a leading cause of disability. Treatment adherence is a critical unmet need; approximately 40–50% of schizophrenia patients are non-adherent to oral antipsychotics, leading to relapse, hospitalization, and poor functional outcomes. Long-acting injectable antipsychotics address this challenge by reducing dosing frequency from daily to monthly or longer intervals, thereby improving treatment continuity and clinical stability.
Paliperidone palmitate occupies a significant position in the long-acting injectable antipsychotic market. Its D2 dopamine antagonism combined with 5-HT2a antagonism provides a balanced neurochemical profile associated with efficacy across positive and negative symptoms. The intramuscular route bypasses first-pass metabolism, enabling predictable pharmacokinetics and sustained therapeutic levels.
Commercially, the antipsychotic market remains substantial despite generic competition for oral formulations. Long-acting injectables command premium pricing due to manufacturing complexity and clinical value. Janssen's portfolio includes both oral (INVEGA) and injectable (paliperidone palmitate) formulations, enabling a tiered treatment strategy. The competitive landscape includes established agents such as aripiprazole (ABILIFY), risperidone, olanzapine, and lurasidone, as well as emerging alternatives like brexpiprazole (REXULTI). Paliperidone palmitate's regulatory approvals across the US, EU, and Australia position it as a mature, widely-available option for clinicians managing treatment-resistant or non-adherent populations.
Drug Class: Atypical antipsychotic (second-generation antipsychotic)
Mechanism of Action: Dopamine D2 receptor antagonist and serotonin 5-HT2a receptor antagonist
Modality: Small molecule
Route of Administration: Intramuscular injection (depot formulation)
Target: D2 dopamine receptor (primary); 5-HT2a serotonin receptor (secondary)
Therapeutic Class: Nervous system agents (ATC N05)
Related Therapies: Oral paliperidone (INVEGA brand), aripiprazole, risperidone, olanzapine, lurasidone, brexpiprazole
Formulation Strategy: Paliperidone palmitate is the long-chain fatty acid ester of paliperidone, enabling sustained-release kinetics when administered intramuscularly. This formulation reduces dosing frequency and improves medication adherence compared to daily oral therapy.
First Approval: Oral paliperidone (INVEGA) was first listed in Australia on 1 April 2008. Paliperidone palmitate received US FDA approval (NDA022264) and has subsequently been approved in the EU and other major markets.
Patent Status: Not yet 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).
Oral paliperidone (INVEGA) approved in Australia
TGA approval of INVEGA oral formulation marks initial regulatory authorization for the paliperidone molecule in a major market.
Phase 3 development completed
Paliperidone palmitate program completes Phase 3 clinical development; regulatory status already established in US, EU, and Australia.
Paliperidone palmitate competes within a mature antipsychotic market dominated by multiple therapeutic classes and formulation strategies. Key competitors include aripiprazole (ABILIFY, Alphapharm/multiple sponsors), which shares the 5-HT2a antagonist mechanism and is available in both oral and long-acting injectable formulations; brexpiprazole (REXULTI, Amneal Pharma Europe), a newer dopamine partial agonist; and risperidone generics (APO-RISPERIDONE, Servier), which employ 5-HT2c antagonism. Olanzapine (APO-OLANZAPINE ODT, Alphapharm) and lurasidone (APO-LURASIDONE, Alphapharm) represent alternative dopamine antagonists with distinct side-effect profiles.
Paliperidone palmitate's competitive advantage lies in its established long-acting injectable formulation, which directly addresses medication adherence—a critical clinical problem in schizophrenia management. Unlike oral formulations, the intramuscular depot delivery ensures sustained therapeutic levels and reduces relapse risk associated with missed doses. The drug's balanced D2/5-HT2a antagonism provides efficacy across positive and negative symptoms, positioning it favorably against dopamine-selective agents.
However, the market also includes non-antipsychotic agents such as zaleplon (SONATA, Teva; GABA-A modulator) and melatonin receptor agonists (HETLIOZ, Vanda), which address specific symptom clusters or comorbidities. Generic competition for oral paliperidone and other antipsychotics has intensified, with multiple US manufacturers (Accord, Mylan/Viatris, PharmScience, Tolmar) now producing paliperidone palmitate generics. This commoditization pressures pricing but expands patient access.
| Therapy | Company | Mechanism | Status |
|---|---|---|---|
| ABILIFY | Alphapharm Pty Ltd | Serotonin 2a (5-HT2a) receptor antagonist | approved |
| REXULTI | Amneal Pharma Europe Ltd | Serotonin 2a (5-HT2a) receptor antagonist | approved |
| SONATA | Teva Pharma GmbH | GABA A receptor alpha-1/beta-1/gamma-2 positive allosteric modulator | approved |
| HETLIOZ | Vanda Pharmaceuticals Netherlands B.V. | Melatonin receptor agonist | approved |
| APO-RISPERIDONE | Servier Laboratories (Aust.) Pty. | Serotonin 2c (5-HT2c) receptor antagonist | approved |
| APO-OLANZAPINE ODT | Alphapharm Pty Ltd | D2-like dopamine receptor antagonist | approved |
| FANAPTUM | Vanda Pharmaceuticals Netherlands B.V. | Dopamine D2 receptor antagonist | approved |
| SAPHRIS | Organon Pharma Pty Ltd | Serotonin 2a (5-HT2a) receptor antagonist | approved |
| ADASUVE | — | Serotonin 2a (5-HT2a) receptor antagonist | approved |
| PFIZER AUSTRALIA PTY LTD | Pfizer Australia Pty Ltd | GABA-A receptor; anion channel positive allosteric modulator | approved |
| BYFAVO | — | GABA-A receptor; anion channel positive allosteric modulator | approved |
| APO-LURASIDONE | Alphapharm Pty Ltd | Dopamine D2 receptor antagonist | 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.
United States: Paliperidone palmitate approved via NDA022264 (Janssen Pharms), NDA207946, and NDA216352. Multiple generic applications (ANDA210397, ANDA211995, ANDA215682, ANDA216228, ANDA216674) approved from Accord Healthcare, Mylan Pharmaceuticals/Viatris, PharmScience, and Tolmar, indicating mature market with established generic competition.
European Union: Authorized as of 19 July 2024 under EMEA/H/C/000746 (Janssen-Cilag International N.V.), EMEA/H/C/002105, EMEA/H/C/004066, EMEA/H/C/005486, and EMEA/H/C/006185. Multiple marketing authorization holders (Janssen-Cilag International NV, Neuraxpharm Pharmaceuticals S.L.) indicate generic or licensed versions in circulation.
Australia: TGA-approved since 1 April 2008 (Janssen-Cilag Pty Ltd). Multiple PBS listings (codes 11066K, 11072R, 11085K, 11094X, 13046P, 13053B, 5100K, 5102M, 5103N, 5107T) reflect various formulation strengths and reimbursement categories. Additional approvals on 1 December 2011 and 1 April 2017 indicate label expansions or new presentations.
Japan (PMDA): Regulatory status not yet disclosed.
China (NMPA): Regulatory status not yet disclosed.
Expected Loss of Exclusivity: Not yet disclosed.
Paliperidone palmitate is an antipsychotic medication approved for the treatment of schizophrenia. It is administered as a long-acting intramuscular injection to improve medication adherence and reduce relapse risk in patients with schizophrenia.
Paliperidone palmitate works by antagonizing dopamine D2 receptors and serotonin 5-HT2a receptors in the brain. This dual mechanism reduces positive symptoms (hallucinations, delusions) and negative symptoms (social withdrawal, apathy) of schizophrenia.
Yes, paliperidone palmitate is FDA-approved. It was approved under NDA022264 (Janssen Pharms) and NDA207946 and NDA216352. Multiple generic versions have also received FDA approval (ANDA210397, ANDA211995, ANDA215682, ANDA216228, ANDA216674).
Yes, paliperidone palmitate is approved in the European Union. It was authorized on 19 July 2024 under multiple EMEA product numbers (EMEA/H/C/000746, EMEA/H/C/002105, EMEA/H/C/004066, EMEA/H/C/005486, EMEA/H/C/006185) with multiple marketing authorization holders.
Yes, paliperidone palmitate is approved in Australia by the TGA. It has been approved since 1 April 2008 and is listed on the PBS with multiple codes (11066K, 11072R, 11085K, 11094X, 13046P, 13053B, 5100K, 5102M, 5103N, 5107T) for various formulation strengths.
Janssen Cilag International NV is the original developer and sponsor. Multiple generic manufacturers now produce paliperidone palmitate, including Accord Healthcare, Mylan Pharmaceuticals/Viatris, PharmScience, and Tolmar in the United States.
Paliperidone palmitate is administered as a long-acting intramuscular injection. This depot formulation provides sustained therapeutic levels over extended periods, reducing the need for daily oral dosing.
Two Phase 3 clinical trials (NCT01051531 and NCT01606254) were conducted to support the development of paliperidone palmitate. Detailed results and trial designs are not yet disclosed in available sources.
Paliperidone palmitate has completed Phase 3 clinical development as of October 2024. The program is mature with established regulatory approvals in the US, EU, and Australia.
Key competitors include aripiprazole (ABILIFY), brexpiprazole (REXULTI), risperidone, olanzapine, and lurasidone. These agents share similar mechanisms (dopamine and serotonin antagonism) and are available in both oral and some cases long-acting injectable formulations.
Paliperidone is the active moiety; paliperidone palmitate is a long-chain fatty acid ester of paliperidone that enables sustained-release kinetics when injected intramuscularly. Oral paliperidone (INVEGA) requires daily dosing, while the palmitate formulation is administered as a monthly or longer-interval injection.
Yes, multiple generic versions of paliperidone palmitate are available in the United States, manufactured by Accord Healthcare, Mylan/Viatris, PharmScience, and Tolmar. These generics have received FDA approval via ANDA applications.
Paliperidone palmitate belongs to the atypical antipsychotic class (second-generation antipsychotics) and is classified under the nervous system therapeutic category (ATC N05).
Paliperidone is a dopamine D2 receptor antagonist and serotonin 5-HT2a receptor antagonist. This dual antagonism reduces both positive symptoms (hallucinations, delusions) and negative symptoms (apathy, social withdrawal) of schizophrenia.
Oral paliperidone (INVEGA) was first approved in Australia on 1 April 2008 by the TGA. It has since received regulatory approvals in multiple other jurisdictions including the US and EU.
Paliperidone palmitate addresses a critical clinical need for improved medication adherence in schizophrenia patients. Long-acting injectable antipsychotics command premium pricing and represent a significant market segment, though generic competition has intensified in recent years.
Paliperidone palmitate → Drug → Target → Indication → Company → Trials → Competitors
Strategic Positioning: Janssen maintains a comprehensive paliperidone portfolio spanning oral (INVEGA) and long-acting injectable (paliperidone palmitate) formulations, enabling a tiered treatment strategy from first-line oral therapy to long-acting depot for adherence-challenged patients. This dual-formulation approach maximizes market penetration and patient access across disease severity and treatment stage.
Competitive Implications: The completion of Phase 3 development and established regulatory approvals across major markets (US, EU, Australia) indicate paliperidone palmitate is a mature, commercially-available product. Generic competition from multiple manufacturers (Accord, Mylan/Viatris, PharmScience, Tolmar) has commoditized the market, reducing branded pricing power but expanding access. Janssen's competitive position depends on brand loyalty, clinical evidence, and integrated care programs rather than patent exclusivity.
Market Dynamics: Long-acting injectable antipsychotics remain clinically valuable despite generic competition because they address a genuine adherence need. Paliperidone palmitate competes against aripiprazole (ABILIFY) long-acting injectables and risperidone microsphere formulations. The market is mature but stable, with demand driven by schizophrenia prevalence, treatment guidelines favoring long-acting agents for non-adherent patients, and healthcare system incentives for reducing relapse-related hospitalizations.
Future Catalysts: Label expansions (e.g., bipolar disorder, other psychotic disorders) could broaden the patient population. Real-world evidence studies demonstrating superior adherence and clinical outcomes versus oral therapy or competing injectables may strengthen market position. Regulatory approvals in emerging markets (Japan, China) would expand geographic reach. Combination therapy data (e.g., with mood stabilizers or anxiolytics) could support new indications.
Unmet Needs: Despite long-acting formulations, approximately 30–40% of patients remain non-adherent to injectable therapy. Development of ultra-long-acting formulations (quarterly or annual dosing) or novel delivery systems (subcutaneous, oral sustained-release) represents a future opportunity. Personalized medicine approaches (pharmacogenomic-guided dosing) could optimize outcomes.
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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.