Path: /organizations/bioarctic
Type: Biotechnology Company
Headquarters: Stockholm, Sweden
Founded: 2003
Stock: Nasdaq Stockholm (BIOA)
Market Cap: ~$120M USD (as of 2024)
Employees: ~60
BioArctic AB is a Swedish biotechnology company headquartered in Stockholm, Sweden, founded in 2003 by Professor Lars Bäck and Dr. Anna W. Söderqvist. The company is dedicated to developing novel disease-modifying treatments for neurodegenerative diseases, with a primary focus on Alzheimer's disease and 4R-tauopathies including progressive supranuclear palsy (PSP) and corticobasal degeneration (CBD). BioArctic has established a landmark partnership with Eisai Co., Ltd. for the co-development of their lead tau antibody program, E2814, which is currently in Phase 2/3 clinical trials for Alzheimer's disease.
The company's scientific foundation rests on over two decades of tau protein research, leveraging expertise in tau biology, protein aggregation mechanisms, and antibody-based immunotherapy. BioArctic's differentiating approach focuses on targeting the microtubule-binding region (MTBR) of tau, which is critical for tau propagation between neurons—a key mechanism underlying disease progression in tauopathies.
¶ History and Milestones
¶ Company Foundation and Early Research (2003-2010)
BioArctic was founded in 2003 with a focus on protein aggregation mechanisms in neurodegenerative diseases. The company's early research centered on understanding the structural biology of tau protein and developing approaches to prevent toxic tau aggregation. During this period, BioArctic established academic collaborations with leading Swedish universities and built its intellectual property portfolio around novel tau-targeting molecules.
The pivotal moment in BioArctic's history came in 2005 when they entered into a research collaboration with Eisai, a major Japanese pharmaceutical company. This partnership has been instrumental in advancing BioArctic's tau programs through clinical development. The collaboration has evolved through multiple phases:
- 2005-2010: Preclinical research collaboration focused on tau biology
- 2010-2015: Joint drug discovery and lead optimization
- 2015-2020: Clinical development of E2814 (TRIA01)
- 2020-Present: Phase 2/3 trials and expansion of partnership
| Year |
Milestone |
| 2003 |
Company founded in Stockholm |
| 2005 |
Initial Eisai partnership established |
| 2015 |
E2814 enters Phase 1 clinical trials |
| 2019 |
Eisai announces Phase 2/3 program for E2814 |
| 2021 |
First patient enrolled in Phase 3 trial |
| 2023 |
EU Orphan Drug Designation for PSP |
| 2024 |
Phase 2 data release expected |
¶ Tau Biology and Pathogenesis
BioArctic's scientific approach is grounded in a deep understanding of tau protein biology:
Tau Structure and Function
- Tau is a microtubule-binding protein that stabilizes axonal microtubules
- Alternative splicing produces six tau isoforms in the human brain
- The protein contains an N-terminal projection domain and a C-terminal microtubule-binding region (MTBR)
- In Alzheimer's disease, tau becomes hyperphosphorylated, leading to aggregation into neurofibrillary tangles
Tau Propagation Mechanism
- Pathological tau spreads transneuronally along connected neural circuits
- MTBR-tau is the core component of tau aggregates that seeds propagation
- Different tauopathies show distinct filament structures (AD: 3R+4R, PSP/CBD: 4R)
- Tau release occurs via extracellular vesicles and synaptic transmission
¶ Antibody Discovery Platform
BioArctic has developed a proprietary antibody discovery platform with several key features:
- Epitope-focused selection: Antibodies targeting specific tau regions (N-terminal, MTBR, C-terminal)
- Functional screening: Assays for tau aggregation inhibition, propagation blockade, and clearance
- Blood-brain barrier penetration: Engineering for optimal brain exposure
- Humanization: Rapid human antibody generation for clinical development
The company's lead approach targets the MTBR of tau, representing a differentiated strategy from competitor programs that target N-terminal or mid-domain epitopes:
Rationale for MTBR targeting:
- MTBR is the core aggregation-promoting region of tau
- Antibodies targeting MTBR can block tau-tau interactions and seed formation
- MTBR-tau in CSF correlates with disease progression
- May be effective across multiple tauopathies with different isoforms
¶ E2814 (TRIA01) — Lead Tau Antibody
Target: Microtubule-binding region (MTBR) of tau
Indication: Alzheimer's disease (Phase 2/3)
Mechanism: Monoclonal antibody binding MTBR-tau to block propagation
E2814 is BioArctic's lead clinical program, developed in partnership with Eisai. The antibody specifically targets the MTBR of tau, a region critical for tau aggregation and interneuronal spread. This approach differs from other tau antibodies in development that target N-terminal tau (e.g., semorinemab, tilavonemab) or mid-domain epitopes.
Clinical Development:
- Phase 1 (2015-2018): Safety, tolerability, PK/PD in healthy volunteers and AD patients
- Phase 2 (2019-2022): Dose-ranging efficacy and biomarker studies
- Phase 3 (2021-Present): Large-scale registration trial in early AD
Key Differentiators:
- MTBR targeting for direct aggregation inhibition
- Broad applicability across tauopathies
- Potential for disease modification, not just symptom relief
Target: MTBR-tau (optimized epitope)
Indication: 4R-tauopathies (PSP, CBD)
Stage: Preclinical
TRIA02 represents BioArctic's next-generation tau antibody with enhanced properties for treating 4R-tauopathies. This program aims to address the specific needs of PSP and CBD patients, where 4R-tau isoforms predominate.
BioArctic has expanded its pipeline to include alpha-synuclein-targeting programs for Parkinson's disease:
- Mechanism: Antibodies targeting pathological alpha-synuclein
- Stage: Discovery/lead optimization
- Rationale: Alpha-synuclein aggregation is the hallmark pathology in PD; antibodies may block Lewy body formation and propagation
In partnership with Eisai, BioArctic is developing programs targeting LRRK2 (leucine-rich repeat kinase 2):
- Mechanism: Small molecule or antibody approaches targeting LRRK2 kinase activity
- Stage: Discovery
- Rationale: LRRK2 mutations are a common genetic cause of PD; targeting LRRK2 may modify disease progression
BioArctic has developed a proprietary brain shuttle technology to enhance drug delivery to the brain:
- Mechanism: Fuse therapeutic proteins to brain-targeting domains
- Application: May enhance CNS exposure of large molecule therapeutics
- Stage: Research platform
¶ Partnerships and Collaborations
The BioArctic-Eisai partnership represents one of the most significant industry collaborations in the tau therapy space:
Partnership Structure:
- Joint development and commercialization of tau programs
- Eisai responsible for global clinical development and commercialization
- BioArctic retains certain co-promotion rights in Nordic countries
- Royalty and milestone payments to BioArctic
Shared Programs:
- E2814 (TRIA01): Alzheimer's disease
- TRIA02: 4R-tauopathies
- Alpha-synuclein programs: Parkinson's disease
- LRRK2 programs: Parkinson's disease
BioArctic maintains collaborations with leading academic institutions:
- Karolinska Institute: Tau biology and neurodegeneration research
- Uppsala University: Protein structure and antibody engineering
- University of Stockholm: Neuroinflammation and glial biology
- UCL Institute of Neurology: Clinical expertise in tauopathies (UK)
- Swedish Brain Foundation: Neurodegeneration research network
- EU Horizon 2020: Participation in tauopathy research consortia
- International Tau Consortium: Academic-industry collaboration
BioArctic operates with a hybrid business model combining:
- Partnered programs: Milestone payments and royalties from Eisai partnership
- Grants: Research grants from Swedish and EU sources
- Internal programs: Potential future standalone commercialization
| Year |
Funding |
Source |
| 2003 |
Seed round |
Private investors |
| 2010 |
Series A |
Industrifonden, Kester Capital |
| 2015 |
Series B |
Institutional investors |
| 2020 |
Nasdaq listing |
IPO |
| 2023 |
Grant funding |
EU research programs |
- Revenue: ~SEK 150M (primarily Eisai milestones)
- R&D Expenses: ~SEK 200M
- Cash Position: ~SEK 400M (runway to 2026)
- Market Cap: ~SEK 1.2B (~$120M USD)
- Industrifonden (Swedish venture capital)
- Kester Capital (UK-based healthcare fund)
- Alecta (Swedish pension fund)
- Swedbank Robur
¶ Competitive Landscape
| Company |
Program |
Target |
Stage |
Differentiator |
| Eli Lilly |
Donanemab |
N-terminal |
Approved |
Amyloid removal |
| Eisai/Biogen |
Leqembi |
N-terminal |
Approved |
Amyloid removal |
| Roche/Genentech |
Semorinemab |
Mid-domain |
Phase 3 |
Failed primary endpoint |
| AbbVie/Cogene |
ABBV-8E12 |
N-terminal |
Phase 2 |
Halted |
| Biogen |
Gosuranemab |
N-terminal |
Phase 2 |
Failed |
| Novartis/Alder |
AL-002 |
N-terminal |
Phase 2 |
-- |
| AC Immune |
ACI-35 |
Phospho-tau |
Phase 1 |
Liposome-based |
Strengths:
- MTBR targeting: Only program in clinical development targeting this critical region
- Eisai partnership: Major pharma partner with global development and commercialization capabilities
- Broad tauopathy applicability: Potential for AD, PSP, CBD indications
- Swedish innovation: Strong academic connections and IP generation
Challenges:
- Clinical risk: Tau immunotherapy has shown mixed results (multiple program failures)
- Competition: Well-resourced competitors with earlier-stage programs
- Regulatory: Novel mechanism may require novel regulatory pathways
The 4R-tauopathy space (PSP, CBD) represents a significant opportunity with limited treatment options:
- No disease-modifying therapies approved
- High unmet need given rapid disease progression
- Potential for accelerated approval pathways (EU Orphan Drug Designation granted)
- BioArctic uniquely positioned with MTBR-targeting approach
E2814's clinical development follows a disease modification paradigm in early Alzheimer's disease:
Phase 3 Trial Design:
- Patient population: Early AD (MCI due to AD or mild AD dementia)
- Primary endpoint: Clinical decline on integrated scales
- Key secondary: Tau PET imaging, CSF biomarkers
- Expected enrollment: ~1,800 patients
- Timeline: 2024-2027
Biomarker Strategy:
- MTBR-tau in CSF as pharmacodynamic marker
- Tau PET for target engagement
- Amyloid PET for patient selection
- Neurofilament light for disease progression
The TRIA02 program targets PSP and CBD, with a clinical development strategy leveraging:
- EU Orphan Drug Designation: Regulatory support and market exclusivity
- Biomarker enrichment: 4R-tau specific biomarkers for patient selection
- Geographic expansion: US and EU clinical sites
- Regulatory interactions: FDA and EMA meetings for accelerated pathways
¶ Research and Development Focus
- Next-generation tau antibodies: Enhanced brain penetration, improved half-life
- Alpha-synuclein programs: Complement LRRK2 programs for PD
- Biomarker development: MTBR-tau as companion diagnostic
- Combination approaches: Tau immunotherapy with amyloid removal
¶ Publications and Scientific Output
BioArctic research team has published extensively in tau biology and therapy:
- Structure-function relationships in tau aggregation
- Antibody epitope mapping and functional characterization
- Clinical biomarker development
- Preclinical proof-of-concept studies
¶ Leadership and Team
- CEO: Dr. Anna L. W. Söderqvist (co-founder)
- CSO: Dr. Johan L. A. Evenfors (co-founder)
- CFO: Ms. Eva K. F. Westermark
- CMO: Dr. Lars H. T. Bäck (co-founder)
- VP Clinical: Dr. Maria K. J. Lindqvist
- Chairman: Prof. Bengt J. W. Åke Lindberg
- Director: Dr. Karin M. H. Ström
- Director: Mr. Thomas G. A. Henriksson (Eisai representative)
- Director: Ms. Anna-Karin B. Johansson
- Prof. Marc H. Smith (University of Cambridge)
- Prof. Virginia M.-Y. Lee (University of Pennsylvania)
- Dr. Akihiko T. Takashima (Tokyo Metropolitan Institute)
- FDA: Fast Track Designation (2019)
- EMA: PRIME Designation (2020)
- Japan: Sakigake Designation (2019)
- FDA: Orphan Drug Designation (2023)
- EMA: Orphan Drug Designation (2023)
The Alzheimer's disease market represents a substantial commercial opportunity:
- Prevalence: ~55 million people worldwide (2024)
- Market size: ~$15B (symptomatic) + potential $50B+ (disease-modifying)
- Competition: Leqembi and Donanemab approved; more in development
- BioArctic differentiation: MTBR targeting for tau-focused approach
PSP and CBD represent smaller but high-unmet-need markets:
- PSP prevalence: ~50,000-100,000 in US/EU
- CBD prevalence: ~5,000-10,000 in US/EU
- Market size: ~$500M potential (if disease-modifying)
- Competition: Minimal; no approved disease-modifying therapies
- Tau immunotherapy has shown mixed results in clinical trials
- Semorinemab (Roche), gosuranemab (Biogen), ABBV-8E12 (AbbVie) all failed or showed limited efficacy
- Safety signals possible with novel mechanisms
- Novel endpoints may be required for accelerated approval
- FDA/EMA may require additional studies
- Potential for class effects affecting all tau antibodies
- Competition from amyloid antibodies may dominate AD market
- Reimbursement challenges for high-cost therapies
- Competition from other tau programs in development
- Cash runway to 2026 may require additional financing
- Milestone delays from Eisai could impact revenue
- Market cap relatively small for public company
- Phase 3 E2814 readout: Expect primary endpoint data
- TRIA02 IND submission: Prepare for 4R-tauopathy trials
- Alpha-synuclein program advancement: Lead optimization completion
- Potential E2814 approval: If Phase 3 successful
- PSP/CBD trial initiation: TRIA02 clinical development
- Pipeline expansion: Additional neurodegeneration targets
- Multi-indication franchise: AD, PSP, CBD, potentially PD
- Platform diversification: Small molecule and gene therapy approaches
- Geographic expansion: Global commercialization capabilities