Gosuranemab (BIIB092) - Anti-Tau Antibody Trial in Progressive Supranuclear Palsy
Overview
Mermaid diagram (expand to render)
Gosuranemab (formerly BIIB092) is an anti-tau monoclonal antibody developed by Biogen that targets extracellular [tau protein](/proteins/tau). The drug was evaluated in a Phase 2 clinical trial for Progressive Supranuclear Palsy (PSP) but was terminated due to lack of efficacy["@clinicaltrialsgov"]. This trial represents one of the most significant failures in the anti-tau antibody field and provides critical lessons for future therapeutic development in tauopathies.
| Parameter | Value |
|-----------|-------|
| NCT Number | NCT03068468 |
| Phase | Phase 2 |
| Status | TERMINATED (2019) |
| Sponsor | Biogen |
| Mechanism | Anti-tau monoclonal antibody (N-terminal tau) |
| Target | Extracellular tau protein |
| Population | PSP patients (Richardson syndrome) |
Background and Rationale
Tau Pathology in PSP
PSP is a 4R-tauopathy characterized by the accumulation of hyperphosphorylated 4-repeat tau isoforms in neurofibrillary tangles, tufted astrocytes, and coiled bodies in subcortical and brainstem structures[@boxer2021]. The [tau protein](/proteins/tau) plays a central role in disease pathogenesis, making it an attractive therapeutic target.
Gosuranemab was designed based on the hypothesis that extracellular tau—released from dying neurons—mediates prion-like spreading of pathology throughout the brain[@yamada2011]. The antibody was intended to:
Bind extracellular tau in the brain interstitial fluid
Prevent neuronal uptake of pathological tau
Neutralize toxic tau species before they can spread between neurons
Enhance clearance of extracellular tau via microglial engagementThis approach differed from intracellular-targeting strategies and represented a novel mechanistic hypothesis for disease modification in tauopathies.
Trial Design
Study Architecture
The Phase 2 trial employed a randomized, double-blind, placebo-controlled design:
- Enrollment: Approximately 450 patients with probable PSP
- Arms: Multiple dose cohorts (placebo, low dose, high dose)
- Duration: 52 weeks
- Primary Endpoint: Change in PSP Rating Scale (PSPRS) score
- Secondary Endpoints: Clinical measures, biomarker endpoints
Target Engagement Biomarkers
The trial included biomarker assessments to evaluate target engagement:
- CSF total tau and phospho-tau measurements
- Plasma tau levels
- PET imaging with tau ligands (flortaucipir)
Trial Results
Primary Outcome
The Phase 2 trial in PSP was terminated early after interim analysis showed that the primary endpoint was unlikely to be met[@clinicaltrialsgov]. The trial failed to demonstrate significant clinical benefit compared to placebo:
- No statistically significant difference in PSPRS decline between treatment and placebo arms
- Substantial placebo response confounded interpretation
- Disease progression continued at similar rates regardless of treatment
Biomarker Findings
The biomarker data revealed important insights:
- Modest reduction in CSF tau was observed at higher doses, but this did not correlate with clinical benefit
- Plasma tau showed dose-dependent reduction, but the clinical significance remained unclear
- No clear relationship between biomarker changes and clinical outcomes
Deep Dive: Why It Failed
1. Timing Hypothesis: Too Little, Too Late
The most widely cited explanation for failure relates to disease stage[@fotuhi2019]:
- Established pathology: By the time patients present with PSP symptoms, substantial tau pathology has already accumulated in the brainstem and subcortical structures
- Neurodegeneration threshold: Significant neuronal loss may have already occurred, making reversal impossible
- Compensatory mechanisms exhausted: The brain's ability to compensate for tau-induced dysfunction may be depleted
Implication: Future trials may need to target pre-symptomatic or prodromal populations where tau pathology is more limited.
2. Target Engagement Limitations
Several factors may have limited adequate target engagement[@sigurdsson2019]:
- Blood-brain barrier penetration: Antibody therapeutics face challenges crossing the BBB; CNS exposure may have been insufficient
- Distribution kinetics: Antibody distribution in brain parenchyma is limited compared to small molecules
- Extracellular space access: While gosuranemab targets extracellular tau, the majority of pathological tau exists intracellularly
- Epitope selection: The N-terminal targeting may not efficiently capture the most pathogenic tau species
Implication: Alternative delivery methods (intrathecal, focused ultrasound) or different epitope targets may improve engagement.
The fundamental mechanism hypothesis may have been flawed[@guo2014]:
- Intracellular tau is the driver: Pathological tau primarily exerts its toxic effects inside neurons, where it disrupts microtubule function, causes mitochondrial dysfunction, and triggers synaptic loss
- Extracellular tau may be a consequence: Released tau may represent a cleanup mechanism rather than the primary toxic species
- Antibody cannot reach intracellular space: Therapeutic antibodies cannot access the intracellular compartment where most tau pathology resides
Implication: Intracellular-targeting approaches (ASOs, small molecules) may be more effective than extracellular-targeting antibodies.
4. 4R-Tauopathy Specificity
PSP presents unique challenges compared to Alzheimer's disease[@dickson2010]:
- 4R isoform predominance: Unlike AD (mixed 3R/4R), PSP involves primarily 4R tau, which may have different propagation mechanisms
- Oligodendroglial pathology: PSP involves significant tau pathology in oligodendrocytes (coiled bodies), which may not be accessible to antibody-based therapies
- Different spreading patterns: The anatomical spread of tau in PSP differs from AD, potentially requiring different intervention strategies
Implication: PSP may require different therapeutic approaches than AD; direct tau production reduction (ASOs) may be more appropriate.
5. Biomarker Gaps
The absence of robust biomarkers for target engagement complicated development[@blennow2018]:
- CSF tau as pharmacodynamic marker: While CSF tau decreased, the relationship to actual brain tau reduction remained uncertain
- No PET signal change: Tau PET ligands may not be sensitive enough to detect treatment-induced changes
- Clinical-biomarker disconnect: Biomarker changes did not translate to clinical benefit, raising questions about appropriate endpoints
Implication: Development of better biomarkers for tau biology and treatment response is critical.
6. Trial Design Challenges
PSP-specific trial design issues may have contributed[@boxer2016]:
- Diagnostic heterogeneity: PSP has multiple clinical variants; enrollment may have included patients with other pathologies
- Placebo response: High placebo response rates in neurodegenerative trials complicate signal detection
- Endpoint sensitivity: PSPRS may not be sensitive enough to detect modest disease slowing
- Duration: 52 weeks may be insufficient to observe disease modification
Lessons Learned
For Anti-Tau Antibody Development
Earlier intervention is critical
- Treat patients before substantial neurodegeneration occurs
- Consider enrichment strategies for prodromal or pre-symptomatic populations
- Genetic risk carriers (MAPT mutations) may provide ideal enrollment populations
Improve brain penetration
- Explore active delivery mechanisms (intrathecal, convection-enhanced delivery)
- Consider bispecific antibodies engineered for enhanced BBB crossing
- Use focused ultrasound to transiently open the BBB
Target the right tau species
- Focus on intracellular tau reduction rather than extracellular neutralization
- Consider approaches that reduce all tau isoforms (ASOs, small molecules)
- Target oligomeric and seeded species rather than monomeric tau
Develop better biomarkers
- Establish clear relationships between biomarker changes and brain tau
- Use PET to directly measure treatment effects on tau burden
- Develop assays for specific pathological tau conformations
Refine trial design for PSP
- Use more specific diagnostic criteria (e.g., CSF biomarkers, imaging)
- Consider longer treatment durations
- Employ adaptive designs to identify signals more efficiently
For the Broader Field
The gosuranemab failure contributed to a paradigm shift in tau therapeutic development[@wilcock2019]:
- From antibodies to ASOs: The failure accelerated interest in antisense oligonucleotide approaches (e.g., [BIIB080](/entities/biiib080)) that reduce tau production at the source
- From extracellular to intracellular: Focus shifted toward intracellular targets and tau production reduction
- From symptomatic to disease-modifying: Emphasis on earlier intervention and true disease modification
- From single-target to combination: Recognition that multi-target approaches may be necessary
Comparison with Other Failed Anti-Tau Trials
| Trial | Drug | Mechanism | Outcome | Key Learnings |
|-------|------|-----------|---------|---------------|
| PASSPORT | Gosuranemab | Anti-tau antibody | Failed | Extracellular targeting insufficient |
| NCT02460094 | Tilavonemab | Anti-tau antibody | Failed | Timing, target selection issues |
| NCT02880956 | Semorinemab | Anti-tau antibody | Mixed | Different effects in AD subpopulations |
| NCT03068467 | AbbVie programs | Various | Failed | 4R-tauopathies challenging |
Tau-Lowering ASOs (Current Focus)
The failure of antibody approaches shifted focus to tau-lowering ASOs[@mummery2023]:
- [BIIB080 (MAPTRx)](/entities/biiib080): Reduces tau production at mRNA level, demonstrated 50% CSF tau reduction
- NIO752: Novartis ASO showing proof-of-concept in PSP
- APB-102: Preclinical ASO for 4R-tauopathies
Small Molecule Approaches
Alternative modalities under development:
- Tau aggregation inhibitors: Small molecules preventing tau aggregation
- Tau kinase inhibitors: Targeting tau-phosphorylating enzymes (GSK3β, CDK5)
- Microtubule stabilizers: Supporting neuronal function despite tau pathology
Future Directions
Recommended Trial Designs
Based on lessons from gosuranemab:
Pre-symptomatic enrollment: Target individuals with MAPT mutations or biomarker evidence of tau pathology but no symptoms
Combination approaches: Combine tau reduction with neuroprotective strategies
Personalized medicine: Use biomarkers to select patients most likely to respondUnmet Needs
- Better understanding of tau biology and propagation
- Improved biomarkers for target engagement and response
- Validated animal models reflecting human 4R-tauopathy
- Regulatory pathways for disease-modifying therapies in rare tauopathies
See Also
- [Progressive Supranuclear Palsy](/diseases/progressive-supranuclear-palsy)
- [Tau Protein](/proteins/tau)
- [BIIB080 (MAPTRx) — Tau ASO](/entities/biiib080)
- [Tau Immunotherapy](/therapeutics/tau-immunotherapy)
- [Tauopathies](/mechanisms/tauopathies)
- [4R-Tauopathies](/mechanisms/4r-tauopathies)
References
ClinicalTrials.gov, Study of BIIB092 in Participants With Progressive Supranuclear Palsy (PASSPORT) (n.d.)
[Boxer AL, Yu JT, Golbe LI, et al, New directions in clinical trials for tauopathies (2021)](https://pubmed.ncbi.nlm.nih.gov/33726543/)
[Yamada K, Cirrito JR, Stewart FR, et al, In vivo detection of sporadic and aggregated tau in the human brain (2011)](https://pubmed.ncbi.nlm.nih.gov/21893156/)
[Fotuhi M, M蹄ian V, Szabo P, et al, Time to treatment initiation in neurodegenerative disease: A review of preclinical and clinical evidence (2019)](https://pubmed.ncbi.nlm.nih.gov/31072151/)
[Sigurdsson EM, Tau-focused immunotherapy: A promising strategy for treating Alzheimer's disease and other tauopathies (2019)](https://pubmed.ncbi.nlm.nih.gov/30658743/)
[Guo JL, Lee VM, Cell-to-cell transmission of pathogenic tau proteins in Alzheimer's disease and related tauopathies (2014)](https://pubmed.ncbi.nlm.nih.gov/24252423/)
[Dickson DW, Ahmed Z, Algom AA, et al, Neuropathology of variants of progressive supranuclear palsy (2010)](https://pubmed.ncbi.nlm.nih.gov/20677931/)
[Blennow K, Zetterberg H, The past and future of Alzheimer's disease fluid biomarkers (2018)](https://pubmed.ncbi.nlm.nih.gov/29631380/)
[Boxer AL, Lang AE, Grossman M, et al, Clinical trial designs for progressive supranuclear palsy (2016)](https://pubmed.ncbi.nlm.nih.gov/26969387/)
[Wilcock GK, The future of Alzheimer's disease: A matter of targeting (2019)](https://pubmed.ncbi.nlm.nih.gov/30915461/)
[Mummery CJ, Börjesson-Hanson A, Berber S, et al, Tau-targeting antisense oligonucleotide BIIB080 in Alzheimer's disease: a phase 1b, randomised, placebo-controlled trial (2023)](https://doi.org/10.1038/s41591-023-02326-3)From the [SciDEX Exchange](/exchange) — scored by multi-agent debate
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Related Analyses:
- [4R-tau strain-specific spreading patterns in PSP vs CBD](/analysis/SDA-2026-04-01-gap-005) 🔄
Pathway Diagram
The following diagram shows the key molecular relationships involving Gosuranemab (BIIB092) PSP Trial discovered through SciDEX knowledge graph analysis:
Mermaid diagram (expand to render)