NCT06021197
- Objective
- Not yet disclosed
- Design
- Not yet disclosed
- Participants
- Not yet disclosed
- Primary endpoint
- Not yet disclosed
- Results
- Results not yet reported
pharma · Nasopharyngeal Carcinoma · Hepatocellular Carcinoma
Xiyuan Hospital of China Academy of Chinese Medical Sciences
Chinese Academy of is a pharma organization headquartered in TAIZHOU, CN. Primary therapeutic focus areas include Nasopharyngeal Carcinoma, Hepatocellular Carcinoma, COVID-19, Breast Cancer, Coronary Artery Disease. Nova
Phase 2 · small molecule · Schizophrenia
NMDAE is a small-molecule therapeutic in Phase 2 development for schizophrenia, sponsored by Xiyuan Hospital of China Academy of Chinese Medical Sciences. The program is identified by internal code CMUH114-REC3-042 and is currently active with a latest milestone recorded on 17 September 2025. The mechanism of action an
Internal code CMUH114-REC3-042
NMDAE is a small-molecule therapeutic in Phase 2 development for schizophrenia, sponsored by Xiyuan Hospital of China Academy of Chinese Medical Sciences. The program is identified by internal code CMUH114-REC3-042 and is currently active with a latest milestone recorded on 17 September 2025. The mechanism of action and specific molecular target have not yet been disclosed. Two clinical trials are registered (NCT06021197 and NCT07122895), indicating active patient enrollment or ongoing assessment. As a Phase 2 program, NMDAE remains in the clinical validation stage, with efficacy and safety data being generated to support potential advancement to Phase 3 pivotal trials. The sponsor's strategy appears focused on clinical development within the Chinese regulatory context, given the institutional affiliation with China Academy of Chinese Medical Sciences. Regulatory approval status and projected timelines for advancement have not been disclosed.
Schizophrenia remains a significant unmet medical need globally, affecting approximately 20 million people worldwide with substantial morbidity, mortality, and economic burden. Despite the availability of multiple approved antipsychotics, treatment resistance, tolerability issues, and cognitive dysfunction persist as major clinical challenges. The competitive landscape includes established agents such as clozapine, aripiprazole, paliperidone ER, and iloperidone, as well as emerging therapies like PERSERIS and INTENSIFY SZ. However, these existing treatments do not universally address symptom heterogeneity, side-effect profiles, or the needs of treatment-resistant populations. NMDAE's development in Phase 2 suggests potential differentiation through novel mechanism or improved tolerability, though specific clinical advantages remain undisclosed. The schizophrenia market represents substantial commercial opportunity, particularly in Asia-Pacific regions where NMDAE's sponsor is positioned. Success in Phase 2 could position NMDAE as a competitive option in a market where unmet needs persist despite therapeutic diversity. Patient populations with inadequate response to current therapies or those experiencing dose-limiting adverse effects represent key commercial targets for differentiated antipsychotics.
NMDAE is classified as a small-molecule therapeutic targeting schizophrenia. The specific mechanism of action, molecular target, and route of administration have not been disclosed. The drug represents the small-molecule modality, consistent with the majority of approved antipsychotics in the competitive landscape. Related approved therapies in the schizophrenia space include dopamine antagonists and partial agonists (aripiprazole, paliperidone ER), serotonin-dopamine modulators (iloperidone), and adjunctive agents (valbenazine for tardive dyskinesia, minocycline as augmentation therapy). First approval date and patent status are not yet 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 2 ongoing
NMDAE is actively in Phase 2 development with two registered clinical trials (NCT06021197, NCT07122895) for schizophrenia.
Latest milestone recorded
Most recent program activity milestone documented on 17 September 2025; specific milestone details not yet disclosed.
NMDAE enters a well-established antipsychotic market with multiple approved small-molecule competitors. Clozapine (Bright Minds Biosciences) remains the gold standard for treatment-resistant schizophrenia despite tolerability constraints. Aripiprazole (Otsuka Beijing Research Institute) and paliperidone ER (Hospital Authority, Hong Kong) represent widely-used first- and second-line agents with favorable tolerability profiles. Iloperidone (Vanda Pharmaceuticals) offers serotonin-dopamine modulation. Emerging competitors include PERSERIS (Indivior, long-acting formulation) and INTENSIFY SZ (Disc Medicine), representing innovation in delivery and adjunctive approaches. Adjunctive therapies such as valbenazine (Neurocrine Biosciences) for tardive dyskinesia, minocycline (Bright Minds Biosciences) for augmentation, and vortioxetine (Takeda) for cognitive symptoms reflect the market's focus on addressing treatment-resistant and residual symptoms. NMDAE's competitive positioning depends on its undisclosed mechanism of action and clinical differentiation. Success will require demonstration of superior efficacy, improved tolerability, or efficacy in treatment-resistant populations compared to established agents. The Phase 2 stage provides opportunity to establish clinical proof-of-concept and differentiation before entering the competitive Phase 3 landscape.
| 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.
NMDAE is sponsored by a Chinese institutional entity (Xiyuan Hospital of China Academy of Chinese Medical Sciences), suggesting primary regulatory focus on the National Medical Products Administration (NMPA) in China. FDA, EMA, and PMDA approval status have not been disclosed. The program's Phase 2 status indicates that regulatory interactions and guidance have likely occurred in the sponsor's primary jurisdiction, but formal regulatory pathway designation, breakthrough therapy status, or accelerated development programs are not yet disclosed. No partnership with international regulatory expertise has been identified. Advancement to Phase 3 will require meeting NMPA Phase 2 efficacy and safety benchmarks; international regulatory strategy remains undisclosed.
NMDAE is a small-molecule therapeutic in development for the treatment of schizophrenia. It is currently in Phase 2 clinical trials and has not yet been approved for any indication.
No, NMDAE has not been approved by the FDA. The drug is in Phase 2 development and regulatory approval status has not been disclosed.
The specific mechanism of action for NMDAE has not yet been disclosed by the sponsor. Additional clinical data and publications will be required to understand its molecular target and therapeutic mechanism.
NMDAE is being developed by Xiyuan Hospital of China Academy of Chinese Medical Sciences. The program is identified by internal code CMUH114-REC3-042.
Two clinical trials are registered for NMDAE: NCT06021197 and NCT07122895. Specific trial designs, objectives, and enrollment status have not been disclosed.
NMDAE is in Phase 2 development as of the latest milestone recorded on 17 September 2025. Phase 2 trials are evaluating efficacy and safety in patient populations.
Approved antipsychotics competing in the schizophrenia market include clozapine, aripiprazole, paliperidone ER, iloperidone, and emerging therapies such as PERSERIS and INTENSIFY SZ. Adjunctive therapies include valbenazine and minocycline.
NMDAE's approval timeline has not been disclosed. The drug is currently in Phase 2; Phase 3 initiation and regulatory submission timelines are not yet announced.
Breakthrough therapy designation status for NMDAE has not been disclosed. Such designations are typically announced by regulatory agencies following formal requests from sponsors.
The route of administration (oral, injection, etc.) for NMDAE has not been disclosed. This information will likely be revealed as clinical development progresses.
The specific patient population targeted by NMDAE (treatment-resistant versus treatment-naive) has not been disclosed. Trial designs and inclusion criteria will clarify the intended population.
No international partnership or licensing agreement has been disclosed for NMDAE. The program is currently being developed by the Chinese institutional sponsor.
The specific molecular target for NMDAE has not been disclosed. Understanding the target will be important for assessing its mechanism of action and competitive positioning.
Comparative efficacy and safety data between NMDAE and clozapine are not yet available. NMDAE is in Phase 2 development while clozapine is an approved standard-of-care for treatment-resistant schizophrenia.
Safety data for NMDAE is being collected in Phase 2 trials. Specific adverse event profiles have not yet been disclosed and will be reported upon trial completion.
The geographic scope of NMDAE trials is not yet disclosed. The sponsor's Chinese institutional affiliation suggests primary development in China, but international trial sites may be involved.
NMDAE → Drug → Target → Indication → Company → Trials → Competitors
Strategic Positioning: NMDAE's development by a Chinese institutional sponsor reflects the growing capacity of Chinese research institutions in CNS drug development and the substantial schizophrenia patient population in Asia-Pacific. Phase 2 status with two active trials suggests adequate enrollment and resource commitment.
Competitive Implications: Success in Phase 2 will determine NMDAE's differentiation versus established agents. The undisclosed mechanism of action creates uncertainty regarding competitive advantage. If NMDAE demonstrates efficacy in treatment-resistant populations or superior tolerability, it could capture market share from clozapine or augmentation therapy approaches. Conversely, if efficacy is comparable to existing agents without clear differentiation, market penetration will be limited.
Future Catalysts: Phase 2 efficacy and safety data release will be the critical near-term catalyst. Positive results could trigger Phase 3 initiation and regulatory interactions. Disclosure of mechanism of action and target will enable competitive positioning assessment. International partnership or licensing announcements would signal confidence in development trajectory.
Expected Milestones: Phase 2 completion and data readout are anticipated but not yet scheduled. Phase 3 initiation would represent major de-risking. Regulatory guidance meetings and potential breakthrough designation discussions may occur following Phase 2 data. International regulatory strategy clarification is needed to assess global commercial potential.
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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.