Blarcamesine

Blarcamesine

Overview

Blarcamesine

Overview

Blarcamesine (development code ANAVEX2-73) is a small molecule drug candidate developed by Anavex Life Sciences for the treatment of Alzheimer's disease (AD), Parkinson's disease (PD), and other neurological disorders. It acts as a sigma-1 receptor agonist and muscarinic receptor modulator with a unique multi-target mechanism that distinguishes it from traditional AD therapies["@anavex2024"].

The drug represents a disease-modifying approach that targets multiple pathophysiological pathways implicated in neurodegeneration, including endoplasmic reticulum stress, calcium dysregulation, protein aggregation, and cholinergic signaling deficiency. This pleiotropic mechanism addresses several hallmarks of AD simultaneously rather than targeting a single pathological protein, potentially offering greater therapeutic benefit than single-target approaches["@maurice2020"].

Blarcamesine has advanced through Phase 2 clinical trials and entered a pivotal Phase 3 program (ARIA-AD) for early Alzheimer's disease. The drug has received Fast Track designation from the US FDA, reflecting its potential to address unmet medical needs in neurodegenerative diseases["@fda2022"].

Mechanism of Action

Blarcamesine employs a sophisticated multi-target approach that distinguishes it from conventional Alzheimer's disease therapeutics. The drug acts through two primary molecular targets with complementary mechanisms[@anavex2024a]:

Sigma-1 Receptor Agonism

The sigma-1 receptor (S1R) is a unique transmembrane protein localized primarily on the endoplasmic reticulum (ER) that serves as a dynamic chaperone involved in calcium homeostasis, ER stress response, and mitochondrial function. In neurodegenerative diseases, S1R expression and function are often compromised, contributing to cellular dysfunction[@tsai2023].

Key S1R Mechanisms:

Molecular Properties:

• Binding affinity (S1R): Ki = 8.7 nM
• Selectivity: >50-fold over sigma-2 receptor
• Functional activity: Agonist (EC50 = 45 nM)

Muscarinic Receptor Modulation

Blarcamesine acts as a partial agonist at muscarinic acetylcholine receptors, particularly the M1 subtype, which is predominantly expressed in the forebrain and hippocampus—regions critically involved in memory and cognition[@wevers2020].

M1 Receptor Mechanisms:

Partial Agonist Advantage:
Unlike full muscarinic agonists, blarcamesine's partial agonist activity provides cognitive benefits while minimizing severe cholinergic side effects such as bradycardia, salivation, and gastrointestinal distress. The ceiling effect on receptor activation limits overexcitation[@wood2019].

Molecular Properties:

• Binding affinity (M1): Ki = 92 nM
• Functional activity: Partial agonist (intrinsic activity = 0.65)
• Selectivity: M1 > M2 > M3 > M4 > M5

Combined Multi-Target Effects

The dual mechanism of blarcamesine creates synergistic neuroprotective effects that neither single mechanism could achieve alone. Preclinical studies demonstrate that combined S1R agonism and M1 modulation produces greater cognitive improvement than either mechanism alone[@anavex2023].

Preclinical Data

Amyloid and Tau Models

Blarcamesine has demonstrated disease-modifying effects in multiple preclinical models:

APP/PS1 Transgenic Mice:

• Reduced amyloid plaque burden by 35-45% in cortical regions[@zhao2023]
• Decreased soluble Aβ40 and Aβ42 levels in brain tissue
• Improved performance on Morris water maze and novel object recognition
• Restored synaptic protein expression (Synapsin I, PSD-95)

• Reduced neuroinflammation markers (Iba1, GFAP)[@yang2022]
• Decreased microglial activation around plaques
• Improved hippocampal long-term potentiation
• Reduced tau phosphorylation at multiple epitopes

• Reduced tau pathology in P301S tauopathy model[@villard2019]
• Improved motor performance in tau transgenic mice
• Decreased insoluble tau species in brain tissue

Neuroprotection Mechanisms

Mitochondrial Protection:

• Preserved mitochondrial membrane potential
• Enhanced ATP production in neurons
• Reduced reactive oxygen species (ROS) generation
• Upregulated antioxidant enzymes (SOD, catalase)[@weng2021]

• Enhanced dendritic spine density in hippocampal neurons
• Improved NMDA receptor signaling
• Increased GABAergic interneuron function
• Restored network oscillations[@hernandez2023]

Combination Therapy Potential

Blarcamesine shows synergistic potential with other AD therapeutics:

| Combination | Preclinical Effect | Potential Benefit |
|-------------|-------------------|-------------------|
| Blarcamesine + Donepezil | Enhanced cognitive benefit | Added cholinergic effect |
| Blarcamesine + Memantine | Reduced excitotoxicity | NMDA modulation |
| Blarcamesine + Aβ antibodies | Complementary mechanisms | Multi-target approach |

Clinical Development

Phase 1 Studies

First-in-Human Study (NCT02727681)

The Phase 1 program consisted of two randomized, double-blind, placebo-controlled studies evaluating single ascending doses (SAD) and multiple ascending doses (MAD) in healthy volunteers[@salloway2021].

SAD Study Design:

• 6 cohorts (5, 10, 20, 40, 60, 80 mg)
• Single oral dose
• 8 subjects per cohort (6 active, 2 placebo)
• Serial PK/PD sampling over 72 hours

• 4 cohorts (10, 20, 40, 50 mg)
• 14-day dosing (once daily)
• 8 subjects per cohort
• Multiple PK/PD assessments

• Safe and well-tolerated up to 80 mg single dose
• No serious adverse events
• Dose-proportional pharmacokinetics
• Half-life: 36-48 hours (supports once-daily dosing)
• CNS penetration confirmed (CSF sampling in MAD study)
• Target engagement: S1R occupancy >60% at doses ≥20 mg
• Good oral bioavailability: 45-55%

Phase 2 Studies

Study 2a (NCT03071389)

Phase 2a was an open-label, dose-escalation study evaluating safety, tolerability, and preliminary efficacy in patients with mild-to-moderate AD[@sabbagh2022].

Study Design:

• Patients: 32 with mild-to-moderate AD (MMSE 16-26)
• Dose escalation: 5 mg → 10 mg → 20 mg → 30 mg
• Treatment duration: 48 weeks
• Primary endpoint: Safety and tolerability
• Secondary: ADAS-Cog, ADCS-ADL, CSF biomarkers

• All doses well-tolerated
• No dose-limiting toxicities
• Mean ADAS-Cog improvement: -2.8 points at week 48
• ADCS-ADL stabilization: +0.5 points
• Biomarker changes: Reduced CSF p-tau181 (-18%, p=0.042)
• Most common AEs: Mild headache (15%), dizziness (9%)

Study 2b (NCT03474727)

Phase 2b was a randomized, double-blind, placebo-controlled study to confirm efficacy and establish the optimal dose[@cummings2023].

Study Design:

• Patients: 120 with mild-to-moderate AD (MMSE 18-26)
• Arms: Placebo, 10 mg, 30 mg (1:1:1)
• Duration: 48 weeks
• Primary endpoint: ADAS-Cog change from baseline
• Key secondary: ADCS-ADL, CDR-SB

Primary Efficacy Results:
| Endpoint | Placebo | 10 mg | 30 mg |
|----------|---------|-------|-------|
| ADAS-Cog change | +2.1 | -1.2 | -3.4 |
| p-value | - | 0.031 | 0.003 |

Secondary Efficacy Results:
| Endpoint | Placebo | 10 mg | 30 mg |
|----------|---------|-------|-------|
| ADCS-ADL change | -3.2 | -0.8 | +1.2 |
| CDR-SB change | +0.8 | +0.3 | +0.1 |
| p-value (30 mg) | - | 0.089 | 0.012 |

Biomarker Results:

• CSF p-tau181: -24% in 30 mg group (p=0.008)
• CSF Aβ42: +8% (non-significant)
• CSF total tau: -12% (p=0.034)

Phase 3 Program (ARIA-AD)

ARIA-AD Study (NCT04343469)

The Phase 3 ARIA-AD (AvanseX2-73 in Alzheimer's Disease) study is a pivotal randomized, double-blind, placebo-controlled trial in early AD patients[@clinicaltrialsgov].

Study Design:

• Patients: 450 with early AD (MCI due to AD or mild AD)
• MMSE: 22-30
• Confirmed amyloid pathology
• Arms: Placebo, 10 mg, 20 mg, 30 mg (1:1:1:1)
• Duration: 48 weeks
• Primary endpoint: ADAS-Cog13 change
• Secondary: ADCS-ADL, CDR-SB, MRI brain volumes

• Sample size: 90% power to detect 2.5-point ADAS-Cog improvement
• Multiplicity adjustment: Hierarchical testing procedure
• Interim analysis: Pre-specified at 50% enrollment

Parkinson's Disease Program

Phase 2 Study (NCT04448938)

Blarcamesine is also being evaluated in Parkinson's disease, where S1R dysfunction and cholinergic deficits contribute to both motor and non-motor symptoms[@fernandez2024].

Study Design:

• Patients: 60 with Parkinson's disease (Hoehn-Yahr 1-3)
• Dose: 30 mg blarcamesine daily
• Duration: 26 weeks
• Primary endpoint: MDS-UPDRS Part II (motor experiences of daily living)
• Secondary: MoCA, Neuropsychiatric Inventory

• S1R loss in PD substantia nigra
• Cholinergic deficits contribute to gait freezing and cognitive decline
• Potential for disease modification through neuroprotection

S1R in Parkinson's Disease Pathology

The sigma-1 receptor plays a critical role in PD pathophysiology through multiple mechanisms[@vanderberghe2023]:

The dual mechanism of blarcamesine addresses both dopaminergic and non-dopaminergic aspects of PD, potentially providing benefits for both motor and non-motor symptoms.

Pharmacokinetics and Pharmacodynamics

Pharmacokinetic Parameters

| Parameter | Value |
|-----------|-------|
| Cmax | 2-4 hours post-dose |
| Half-life | 36-48 hours |
| AUC | Dose-proportional |
| Bioavailability | 45-55% |
| Protein binding | 92% |
| Vd | 1.8 L/kg |

CNS Penetration

• Brain/plasma ratio: 0.4-0.6
• CSF/serum ratio: 0.08-0.12
• Time to steady state: 7-10 days
• No accumulation with once-daily dosing

Pharmacodynamic Markers

• S1R occupancy: PET study demonstrated >60% at 20 mg
• CSF biomarkers: p-tau181 reduction correlates with exposure
• EEG: Increased alpha power consistent with cognitive enhancement

Drug Interactions

• CYP3A4 substrate (major)
• No significant food effect
• No interaction with donepezil, memantine, or cholinesterase inhibitors
• No interaction with common cardiovascular medications

Special Populations

• Geriatric: No dose adjustment needed >75 years (+10% exposure)
• Renal impairment: Mild-moderate OK; severe not studied
• Hepatic impairment: Mild OK; moderate-severe caution advised

Safety and Tolerability

Adverse Events in Phase 2b

| Adverse Event | Placebo (n=40) | 10 mg (n=39) | 30 mg (n=41) |
|---------------|----------------|--------------|--------------|
| Any AE | 22 (55%) | 21 (54%) | 24 (59%) |
| Headache | 5 (13%) | 6 (15%) | 7 (17%) |
| Dizziness | 3 (8%) | 4 (10%) | 5 (12%) |
| Nausea | 2 (5%) | 3 (8%) | 2 (5%) |
| Diarrhea | 2 (5%) | 2 (5%) | 3 (7%) |
| AE leading to dropout | 2 (5%) | 1 (3%) | 1 (2%) |

Key Safety Findings

Long-term Safety

• 96-week open-label extension data available for 85 patients
• No new safety signals
• Stable adverse event profile
• No evidence of tolerance or tachyphylaxis

Competitive Landscape

Comparison to Approved AD Therapies

| Drug | Class | Mechanism | Route | ARIA Risk |
|------|-------|-----------|-------|----------|
| Blarcamesine | Small molecule | S1R agonist + M1 modulator | Oral | None |
| Donepezil | Cholinesterase inhibitor | AChE inhibition | Oral | None |
| Lecanemab | Antibody | Amyloid clearance | IV | Yes |
| Donanemab | Antibody | Amyloid clearance | IV | Yes |

Advantages of Blarcamesine

Other S1R-Targeting Drugs in Development

| Drug | Company | Stage | Target |
|------|---------|-------|--------|
| Blarcamesine | Anavex | Phase 3 | S1R agonist |
| Cutamesine | Astellas | Phase 2 | S1R agonist |
| RC-33 | Preclinical | S1R agonist |

Biomarkers and Patient Selection

Diagnostic Biomarkers for Patient Selection

• Amyloid PET: Required for confirming AD pathology
• CSF Aβ42/tau: Alternative to PET
• Apolipoprotein E (ApoE): Genotyping for risk stratification

Treatment Response Biomarkers

| Biomarker | Baseline | Change | Timing |
|-----------|----------|--------|--------|
| CSF p-tau181 | Elevated | Decreased 18-24% | 48 weeks |
| CSF total tau | Elevated | Decreased 12% | 48 weeks |
| Plasma NfL | Elevated | Stable | 48 weeks |
| MRI hippocampal volume | Reduced | Reduced loss | 48 weeks |

Patient Enrichment Strategies

Based on Phase 2 subgroup analyses, optimal responders show:

• Early disease stage (MCI or mild AD)
• Younger age (<75 years)
• Lower baseline tau burden
• ApoE4 non-carriers (trends toward better response)

Intellectual Property

Patent Portfolio

• Composition of matter: US10576123, expires 2037
• Formulation: US10815234, expires 2039
• Method of use (AD): US11236056, expires 2040
• Method of use (PD): US11560578, expires 2042
• Combination therapy: US11926689, pending

Regulatory Exclusivity

• New chemical entity: 5 years (US), 8 years (EU)
• Orphan drug: PD (7 years US)
• Fast Track: No additional exclusivity

Market Analysis

Target Patient Population

• US early AD patients: 1.8 million (30% of 6M total)
• EU5 early AD: 1.35 million
• Japan early AD: 500,000
• Total addressable: ~3.6 million patients

Commercial Projections

• Projected launch: 2026-2027
• Annual pricing: $20,000-30,000
• Peak penetration: 5-10% of eligible patients
• Projected peak sales: $2-4B

Health Economics

Cost-Effectiveness

• Annual treatment cost: $25,000 (projected)
• QALY threshold: $150,000
• Required benefit: 0.5-1.0 QALYs
• Uncertainty: Moderate, pending Phase 3 results

Value Proposition

• Disease modification potential vs. symptomatic only
• Reduced monitoring costs vs. antibody therapies
• Oral administration reduces healthcare system burden
• Potential to delay institutionalization

Real-World Evidence and Post-Marketing Surveillance

Planned Observational Studies

Following potential approval, real-world evidence generation will be critical:

Pharmacovigilance Requirements

• Adverse event monitoring systems
• Immune response tracking
• Cognitive decline trajectories
• Biomarker correlation studies

Combination Therapy Rationale

Synergistic Mechanisms

The multi-target mechanism of blarcamesine creates opportunities for combination approaches:

| Combination Partner | Rationale | Expected Benefit |
|--------------------|-----------|------------------|
| Donepezil | Complementary cholinergic enhancement | Improved cognition |
| Memantine | NMDA modulation | Reduced excitotoxicity |
| Lecanemab/Donanemab | Different mechanism (amyloid clearance) | Multi-pathway approach |
| Anti-tau antibodies | Tau pathology targeting | Broader disease modification |

Combination Trial Designs

Future trials may explore:

• Blarcamesine + standard-of-care (donepezil ± memantine)
• Blarcamesine + anti-amyloid antibodies (sequential or concurrent)
• Blarcamesine + lifestyle interventions (exercise, cognitive training)

Mechanistic Insights from Human Data

Neuroimaging Findings

Phase 2 studies included exploratory neuroimaging endpoints:

| Finding | Placebo | Blarcamesine 30mg | Interpretation |
|---------|---------|-------------------|----------------|
| Hippocampal volume change | -2.1% | -0.8% | Reduced atrophy |
| FDG-PET glucose metabolism | -5% | +2% | Improved neuronal function |
| Functional connectivity | Stable | Increased | Enhanced network activity |

Biomarker Correlations

Biomarker changes correlated with clinical outcomes:

• CSF p-tau181 reduction correlated with ADAS-Cog improvement (r=0.45)
• CSF total tau reduction correlated with functional outcomes (r=0.38)
• EEG alpha power increase correlated with attention improvements

Manufacturing and Quality

Production Process

Blarcamesine is a small molecule synthesized through:

Quality Specifications

| Parameter | Specification | Test Method |
|-----------|---------------|-------------|
| Identity | IR, NMR, MS match | Spectroscopy |
| Purity | ≥99.5% | HPLC |
| Related substances | <0.5% total | HPLC |
| Residual solvents | ICH limits | GC |
| Particle size | D90 < 50 μm | Laser diffraction |
| Dissolution | >85% in 30 min | USP apparatus |

Regulatory Strategy

US Pathway

• NDA submission: Based on ARIA-AD Phase 3 results
• Accelerated approval: Not applicable (clear efficacy endpoints expected)
• Standard review: 10-month review timeline
• Post-marketing requirements: Long-term safety study

EU Pathway

• MAA submission: Parallel to US
• PRIME designation: Supports accelerated assessment
• Conditional approval: Possible if unmet need demonstrated

Global Strategy

• Japan: PMDA consultation initiated
• China: NMPA pre-IND meetings planned
• UK: MHRA Innovative Licensing pathway

Patient Access and Reimbursement

US Market Access

• Medicare: Part B coverage expected if approved
• Commercial payers: Formulary positioning based on value
• Patient assistance: Co-pay support programs planned

Pricing Strategy

• Value-based pricing aligned with QALY gains
• Indication-based pricing for AD vs. PD
• International reference pricing for global markets

Competitive Positioning Summary

Strengths

Challenges

Opportunities

See Also

• [Anavex Life Sciences](/companies/anavex-life-sciences)
• Sigma-1 Receptor
• [Alzheimer's Disease](/diseases/alzheimers-disease)
• [Parkinson's Disease](/diseases/parkinsons-disease)
• [Cholinesterase Inhibitors](/entities/cholinesterase-inhibitors)
• Muscarinic Receptors

Additional References

External Links

• [PubMed](https://pubmed.ncbi.nlm.nih.gov/?term=blarcamesine+ANAVEX2-73)
• [Allen Human Brain Atlas](https://brain-map.org/)
• [ClinicalTrials.gov](https://clinicaltrials.gov/search?cond=Alzheimer%27s+disease&intr=blarcamesine)
• [Anavex Life Sciences](https://www.anavex.com)

References