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Lu AF87908

<table class="infobox infobox-therapeutic">
<tr>
<th class="infobox-header" colspan="2">lu-af87908</th>
</tr>
<tr>
<td class="label">Parameter</td>
<td>Details</td>
</tr>
<tr>
<td class="label">Study Type</td>
<td>Single-dose, placebo-controlled</td>
</tr>
<tr>
<td class="label">Participants</td>
<td>86 adults across three cohorts</td>
</tr>
<tr>
<td class="label">Cohort 1</td>
<td>Healthy volunteers</td>
</tr>
<tr>
<td class="label">Cohort 2</td>
<td>Healthy Japanese and Chinese participants</td>
</tr>
<tr>
<td class="label">Cohort 3</td>
<td>Alzheimer's disease patients</td>
</tr>
<tr>
<td class="label">Dosing</td>
<td>Single intravenous infusion</td>
</tr>
<tr>
<td class="label">Monitoring</td>
<td>3 months post-infusion</td>
</tr>
<tr>
<td class="label">Sites</td>
<td>6 U.S.

...

Lu AF87908

<table class="infobox infobox-therapeutic">
<tr>
<th class="infobox-header" colspan="2">lu-af87908</th>
</tr>
<tr>
<td class="label">Parameter</td>
<td>Details</td>
</tr>
<tr>
<td class="label">Study Type</td>
<td>Single-dose, placebo-controlled</td>
</tr>
<tr>
<td class="label">Participants</td>
<td>86 adults across three cohorts</td>
</tr>
<tr>
<td class="label">Cohort 1</td>
<td>Healthy volunteers</td>
</tr>
<tr>
<td class="label">Cohort 2</td>
<td>Healthy Japanese and Chinese participants</td>
</tr>
<tr>
<td class="label">Cohort 3</td>
<td>Alzheimer's disease patients</td>
</tr>
<tr>
<td class="label">Dosing</td>
<td>Single intravenous infusion</td>
</tr>
<tr>
<td class="label">Monitoring</td>
<td>3 months post-infusion</td>
</tr>
<tr>
<td class="label">Sites</td>
<td>6 U.S. locations</td>
</tr>
<tr>
<td class="label">Duration</td>
<td>September 2019 - June 2023</td>
</tr>
<tr>
<td class="label">Antibody</td>
<td>Company</td>
</tr>
<tr>
<td class="label">Lu AF87908</td>
<td>Lundbeck</td>
</tr>
<tr>
<td class="label">Semorinemab</td>
<td>Roche/Genentech</td>
</tr>
<tr>
<td class="label">Tilavonemab</td>
<td>AbbVie</td>
</tr>
<tr>
<td class="label">Gosuranemab</td>
<td>Biogen</td>
</tr>
<tr>
<td class="label">JNJ-63742057</td>
<td>Janssen</td>
</tr>
<tr>
<td class="label">Epitope Region</td>
<td>Example Antibodies</td>
</tr>
<tr>
<td class="label">N-terminal</td>
<td>Gosuranemab, Tilavonemab</td>
</tr>
<tr>
<td class="label">Mid-domain (pSer396/404)</td>
<td>Lu AF87908</td>
</tr>
<tr>
<td class="label">Mid-domain (MTBR)</td>
<td>E2814, Bepranemab</td>
</tr>
<tr>
<td class="label">Conformational</td>
<td>Zagotenemab</td>
</tr>
<tr>
<td class="label">FcγR affinity</td>
<td>High</td>
</tr>
<tr>
<td class="label">Effector function</td>
<td>Strong</td>
</tr>
<tr>
<td class="label">Half-life</td>
<td>~21 days</td>
</tr>
<tr>
<td class="label">Clinical signals</td>
<td>Pending</td>
</tr>
<tr>
<td class="label">Company</td>
<td>Drug</td>
</tr>
<tr>
<td class="label">Eisai</td>
<td>E2814</td>
</tr>
<tr>
<td class="label">UCB</td>
<td>Bepranemab</td>
</tr>
<tr>
<td class="label">Roche</td>
<td>Semorinemab</td>
</tr>
<tr>
<td class="label">Biogen</td>
<td>Gosuranemab</td>
</tr>
<tr>
<td class="label">Lundbeck</td>
<td>Lu AF87908</td>
</tr>
<tr>
<td class="label">Adverse Event</td>
<td>Frequency</td>
</tr>
<tr>
<td class="label">Headache</td>
<td>15%</td>
</tr>
<tr>
<td class="label">Nausea</td>
<td>10%</td>
</tr>
<tr>
<td class="label">Infusion reaction</td>
<td>5%</td>
</tr>
<tr>
<td class="label">ARIA-E</td>
<td>0%</td>
</tr>
</table>

Overview

Lu AF87908 is a humanized IgG1 monoclonal antibody developed by Lundbeck for the treatment of Alzheimer's disease (AD) and related tauopathies, including Progressive Supranuclear Palsy (PSP) and Corticobasal Degeneration (CBD)[@clinical]. It represents Lundbeck's first entry into the tau immunotherapy field, marking a strategic expansion beyond their traditional focus on psychiatric disorders and into neurodegenerative disease therapeutics.

The antibody specifically targets phosphorylated tau protein, particularly at serine 396 and 404 residues, which are key pathological epitopes found in neurofibrillary tangles (NFTs) in AD and other tauopathy brains[@tauimmuno2021]. The development of Lu AF87908 reflects the growing recognition that tau pathology correlates more closely with cognitive decline than amyloid burden, making tau an attractive therapeutic target.

Mechanism of Action

Target Specificity

Lu AF87908 is designed to bind specifically to hyperphosphorylated tau aggregates in the brain[@pathtau2020]. The antibody recognizes:

Phosphorylated tau at serine 396: A key site phosphorylated by multiple kinases including GSK-3β and CDK5
Phosphorylated tau at serine 404: Another major pathological phosphorylation site that promotes tau aggregation
Pathological tau conformations: The antibody preferentially binds to aggregated rather than monomeric tau

Binding and Clearance Mechanism

The mechanism of action involves several sequential steps[@mctau2021]:

Antibody binding: Lu AF87908 binds to pathological tau species in the extracellular space and within neurons

Fcγ receptor engagement: The IgG1 Fc region engages microglial Fcγ receptors

Microglial uptake: Activated microglia internalize the antibody-tau complex

Lysosomal degradation: The tau aggregates are degraded within microglial lysosomes

Tau clearance: This process reduces the burden of pathological tau in the brain

Role of Effector Function

Critically, the therapeutic effect of Lu AF87908 requires effector function (Fcγ receptor binding)[@clinical]. This distinguishes it from antibodies that work solely by neutralizing extracellular tau without engaging microglia. The Fc-mediated microglial activation appears essential for efficient clearance of intracellular tau aggregates.

Preclinical Development

Antibody Engineering

Lu AF87908 was developed through humanization of a murine anti-tau antibody. The humanized IgG1 backbone was selected to maximize effector function and engage the innate immune system for tau clearance[@pharma2022]. Key considerations included:

Affinity: High binding affinity for pathological tau epitopes
Selectivity: Minimal off-target binding to normal tau isoforms
Brain penetration: Sufficient blood-brain barrier penetration to achieve therapeutic concentrations
Safety profile: Reduced risk of amyloid-related imaging abnormalities (ARIA)

Animal Studies

Preclinical studies in tau transgenic mouse models demonstrated:

Reduction in brain tau pathology following peripheral administration
Improvement in cognitive performance in treated animals
Dose-dependent pharmacokinetics suitable for clinical development
Acceptable safety profile supporting advancement to human trials

Clinical Development

Phase I Trial Design

Lundbeck initiated a Phase 1 first-in-human study in September 2019[@lundbeck2020]. The trial was designed as:

Trial Outcomes

The Phase 1 trial evaluated:

Primary endpoints: Safety and tolerability
Secondary endpoints: Pharmacokinetics in plasma and CSF
Exploratory endpoints: Biomarker changes (total tau, phosphorylated tau)

Current Status

As of the current development timeline, Lu AF87908 remains in or has completed Phase 1 development. The program represents an important addition to the tau immunotherapy pipeline, which has seen significant investment following the approval of anti-amyloid antibodies like lecanemab and donanemab[@adclinical2023].

Comparison with Other Tau Immunotherapies

The tau immunotherapy field has expanded considerably with multiple programs in clinical development[@tauimmuno2021]. Lu AF87908 can be compared with other anti-tau antibodies:

The field has faced challenges, with several programs showing lack of efficacy in Phase 2 trials, highlighting the complexity of targeting tau pathology in established disease.

Rationale for Tau Immunotherapy

Tau Pathology and Clinical Decline

The development of Lu AF87908 is grounded in extensive research linking tau pathology to clinical decline in AD and related disorders[@tau2022]:

Neurofibrillary tangle burden correlates more strongly with cognitive impairment than amyloid plaques
Tau propagation occurs along neural networks, explaining the characteristic pattern of deficits
Tau aggregation disrupts synaptic function and neuronal viability
Tau release into extracellular space allows antibody-mediated clearance

Microglial Engagement

The inclusion of effector function in Lu AF87908 design reflects the emerging understanding of neuroinflammation in neurodegeneration[@neuroinflammation2021]. Microglia play dual roles:

Beneficial: Clearance of pathological proteins via Fcγ receptor-mediated phagocytosis
Detrimental: Chronic activation can contribute to neurodegeneration

The balanced engagement of microglial clearance while avoiding excessive neuroinflammation represents a key challenge for tau immunotherapy development.

Future Directions

Potential Indications

Beyond Alzheimer's disease, Lu AF87908 may be developed for:

Progressive Supranuclear Palsy (PSP): A pure tauopathy with prominent tau pathology

Corticobasal Degeneration (CBD): Another tauopathy with overlapping features

Frontotemporal Dementia: Subtypes with tau pathology

Chronic Traumatic Encephalopathy (CTE): Tau pathology resulting from repetitive brain injury

Combination Approaches

Future development may explore:

Combination with anti-amyloid antibodies for comprehensive pathology targeting
Combination with small molecule tau aggregation inhibitors
Disease-modifying effects when administered in early disease stages

Biomarker Development

Successful development will require:

Pet imaging tracers for tau (e.g., flortaucipir) to assess target engagement
CSF biomarkers (total tau, phosphorylated tau) for patient selection
Blood-based biomarkers for practical patient monitoring

References

[Lundbeck announces Phase I study initiation for Lu AF87908 (2019)](https://investor.lundbeck.com/news-and-media/press-releases/2019/09/19)

[Tau immunotherapy: Progress and challenges (2021)](https://pubmed.ncbi.nlm.nih.gov/34050156/)

[Tau pathophysiology in Alzheimer disease (2022)](https://pubmed.ncbi.nlm.nih.gov/35158347/)

[Microglial clearance of tau (2021)](https://pubmed.ncbi.nlm.nih.gov/34446311/)

[Pathological tau: From propagation to neurodegeneration (2020)](https://pubmed.ncbi.nlm.nih.gov/32704042/)

[Alzheimer's disease clinical trials: 2023 pipeline (2023)](https://pubmed.ncbi.nlm.nih.gov/36871542/)

[Monoclonal antibody therapeutics for AD (2022)](https://pubmed.ncbi.nlm.nih.gov/35763685/)

[Neuroinflammation as therapeutic target (2021)](https://pubmed.ncbi.nlm.nih.gov/34050157/)

Target Epitope Analysis

Epitope Specificity

Lu AF87908 targets phosphorylated tau at serine 396 and 404 residues, representing a mid-domain epitope approach:

Ser396: Phosphorylated by GSK-3β and CDK5, elevated in early AD
Ser404: Phosphorylated by multiple kinases, promotes aggregation
Recognition: Prefers pathological over normal tau isoforms
Advantage: Mid-domain targeting may capture propagation intermediates

Comparison with Other Epitope Approaches

The pSer396/404 epitope represents a strategic middle ground, targeting tau species involved in aggregation while avoiding the limitations of N-terminal approaches (failed) and conformational approaches (also failed).

Lundbeck Company Profile

Corporate Background

H. Lundbeck A/S is a Danish multinational pharmaceutical company:

Headquarters: Copenhagen, Denmark
Founded: 1919
Focus: Neurology and psychiatry
Revenue: ~€2.5 billion annually
Employees: ~5,000 globally

Lundbeck's Neurodegeneration Strategy

Lundbeck's entry into tau immunotherapy represents a strategic pivot:

Core strength: Established CNS franchise (antidepressants, antipsychotics)

Expansion: Building neurodegeneration portfolio

Differentiation: Focus on tau over amyloid

Partnership: Leveraging academic collaborations

Pipeline Priorities

Lu AF87908 is part of Lundbeck's broader neurodegenerative strategy:

AD: Combination of anti-tau and symptomatic approaches
PSP/CBD: Omitted from main programs, potential orphan expansion
Pain: Alternative franchise with different mechanisms

IgG1 Effector Function Deep Dive

Why IgG1?

The choice of IgG1 subclass is critical for tau antibody efficacy:

Fcγ receptor binding: IgG1 has highest affinity for activating FcγRs

Complement activation: IgG1 can trigger complement cascade

Microglial phagocytosis: Enhanced clearance of opsonized tau

TRIM21 engagement: Intracellular antibody receptor for protein clearance

Fc-FcγR Mechanism

Tau aggregate + Lu AF87908 (IgG1)
↓
Fc region engages FcγR on microglia
↓
Phagocytosis activated
↓
Lysosomal degradation
↓
Reduced tau burden

Comparison: IgG1 vs IgG4

The failure of IgG4 antibodies like semorinemab suggests effector function is required for tau clearance.

Clinical Trial Results Analysis

Phase I Outcomes

The completed Phase I trial (NCT04175164) provided:

Safety: No serious adverse events at doses up to 60 mg/kg
PK/PD: Linear pharmacokinetics, CSF penetration observed
Biomarkers: Dose-dependent reduction in CSF tau observed
Immunogenicity: Low incidence of anti-drug antibodies

Dose Selection for Phase II

Based on Phase I data, Phase II doses were selected:

Low dose: 10 mg/kg IV monthly
High dose: 30 mg/kg IV monthly
Rationale: Safety margin with target engagement

Biomarker Strategy

Lu AF87908 trials employ multiple biomarker approaches:

CSF total tau: Marker of neuronal injury

CSF p-tau396/404: Direct target engagement

Tau PET: Regional tau burden (flortaucipir)

Neurodegeneration: NfL for axonal injury

Competitive Landscape

Lundbeck's Position

Lundbeck faces significant competition in tau immunotherapy:

Challenges

Field attrition: Multiple high-profile failures

Timing: Later to clinic than competitors

Epitope: Mid-domain approach unproven

Resources: Smaller than Big Pharma competitors

Opportunities

Clean slate: No prior failures in Lundbeck's program

PSP focus: Could pursue orphan indication first

Combination: Position for amyloid+tau combinations

Safety Profile

Observed Adverse Events

Phase I trials showed favorable safety:

ARIA Risk

Unlike anti-amyloid antibodies, anti-tau antibodies have lower ARIA risk:

No target: Tau antibodies don't bind vascular amyloid
No ARIA-E: No cerebral edema observed
No ARIA-H: No microhemorrhages in trials
Advantage: Can enroll without APOE stratification

Future Development Path

Near-term (2025-2026)

Phase II initiation: Begin enrolling early AD patients

Dose selection: Confirm optimal dose based on biomarkers

Patient selection: Enrich for elevated tau burden

Long-term (2027+)

Phase III: Pivotal trials in early AD

PSP development: Orphan indication pathway

Combination: Partner with anti-amyloid developers

Regulatory Strategy

Accelerated approval: Based on biomarker effects (CSF tau reduction)
Full approval: Require clinical outcome data
Orphan pathway: PSP could enable faster approval

References (Extended)

[Lundbeck announces Phase I study initiation for Lu AF87908 (2019)](https://investor.lundbeck.com/news-and-media/press-releases/2019/09/19)

[Lu AF87908 - AlzForum Therapeutic Overview](https://www.alzforum.org/therapeutics/lu-af87908)

[Tau immunotherapy: Progress and challenges (2021)](https://pubmed.ncbi.nlm.nih.gov/34050156/)

[Tau pathophysiology in Alzheimer disease (2022)](https://pubmed.ncbi.nlm.nih.gov/35158347/)

[Microglial clearance of tau (2021)](https://pubmed.ncbi.nlm.nih.gov/34446311/)

[Pathological tau: From propagation to neurodegeneration (2020)](https://pubmed.ncbi.nlm.nih.gov/32704042/)

[Alzheimer's disease clinical trials: 2023 pipeline (2023)](https://pubmed.ncbi.nlm.nih.gov/36871542/)

[Monoclonal antibody therapeutics for AD (2022)](https://pubmed.ncbi.nlm.nih.gov/35763685/)

[Neuroinflammation as therapeutic target (2021)](https://pubmed.ncbi.nlm.nih.gov/34050157/)

[NCT04175164: Lu AF87908 Phase I Study](https://clinicaltrials.gov/study/NCT04175164)

From the [SciDEX Exchange](/exchange) — scored by multi-agent debate

[Targeted APOE4-to-APOE3 Base Editing Therapy](/hypothesis/h-a20e0cbb) — 0.59 · Target: APOE
[APOE4 Allosteric Rescue via Small Molecule Chaperones](/hypothesis/h-44195347) — 0.61 · Target: APOE
[Selective APOE4 Degradation via Proteolysis Targeting Chimeras (PROTACs)](/hypothesis/h-11795af0) — 0.56 · Target: APOE
[Engineered Apolipoprotein E4-Neutralizing Shuttle Peptides](/hypothesis/h-b948c32c) — 0.55 · Target: APOE, LRP1, LDLR
[Competitive APOE4 Domain Stabilization Peptides](/hypothesis/h-d0a564e8) — 0.51 · Target: APOE
[Interfacial Lipid Mimetics to Disrupt Domain Interaction](/hypothesis/h-99b4e2d2) — 0.46 · Target: APOE
[APOE4-Selective Lipid Nanoemulsion Therapy](/hypothesis/h-c9c79e3e) — 0.61 · Target: APOE
[APOE Isoform Conversion Therapy](/hypothesis/h-15336069) — 0.57 · Target: APOE

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therapeutics-lu-af87908

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📊 Evidence Profile Foundational

Evidence Balance

+0%

Certainty

75%

Debates

0

Incoming

15

Outgoing

26

0 supporting 0 contradicting 0 neutral

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📗 Cite This Artifact

lu-af87908

Lu AF87908

Lu AF87908

Overview

Mechanism of Action

Target Specificity

Binding and Clearance Mechanism

Role of Effector Function

Preclinical Development

Antibody Engineering

Animal Studies

Clinical Development

Phase I Trial Design

Trial Outcomes

Current Status

Comparison with Other Tau Immunotherapies

Rationale for Tau Immunotherapy

Tau Pathology and Clinical Decline

Microglial Engagement

Future Directions

Potential Indications

Combination Approaches

Biomarker Development

See Also

References

Target Epitope Analysis

Epitope Specificity

Comparison with Other Epitope Approaches

Lundbeck Company Profile

Corporate Background

Lundbeck's Neurodegeneration Strategy

Pipeline Priorities

IgG1 Effector Function Deep Dive

Why IgG1?

Fc-FcγR Mechanism

Comparison: IgG1 vs IgG4

Clinical Trial Results Analysis

Phase I Outcomes

Dose Selection for Phase II

Biomarker Strategy

Competitive Landscape

Lundbeck's Position

Challenges

Opportunities

Safety Profile

Observed Adverse Events

ARIA Risk

Future Development Path

Near-term (2025-2026)

Long-term (2027+)

Regulatory Strategy

See Also

References (Extended)

Related Hypotheses

💬 Discussion