nct06544616

JNJ-64042056 (Au-001) - Phosphorylated Tau Active Immunotherapy for Preclinical Alzheimer's Disease

Overview

JNJ-64042056 (Au-001) - Phosphorylated Tau Active Immunotherapy for Preclinical Alzheimer's Disease

Overview

JNJ-64042056 (also known as Au-001) is a phosphorylated tau (p-tau) targeted active immunotherapy being developed by Janssen Pharmaceuticals (Johnson & Johnson) for the prevention of Alzheimer's disease. This Phase 2 clinical trial represents a cutting-edge approach to preventing cognitive decline in individuals at risk for AD before symptoms appear.

The trial is evaluating the efficacy, safety, and immunogenicity of JNJ-64042056 in participants with preclinical Alzheimer's disease — individuals who have evidence of AD pathology (amyloid and/or tau) but do not yet show clinical symptoms of cognitive impairment.

This approach represents a paradigm shift from treating symptomatic AD to preventing or delaying the onset of cognitive impairment in at-risk individuals["@novel2024"][@alzheimers2023].

Trial Details

| Parameter | Value |
|-----------|-------|
| NCT Number | [NCT06544616](https://clinicaltrials.gov/study/NCT06544616) |
| Phase | Phase 2 |
| Status | Active, Not Recruiting |
| Sponsor | Janssen Pharmaceutica N.V., Belgium |
| Enrollment | 498 participants |
| Study Start Date | July 2024 |
| Estimated Completion | July 2032 |
| Indication | Preclinical Alzheimer's Disease |
| Study Type | Interventional |
| Allocation | Randomized, Double-blind, Placebo-controlled |

Mechanism of Action

Phosphorylated Tau as Therapeutic Target

JNJ-64042056 is designed to generate antibodies that specifically target phosphorylated tau (p-tau) proteins. This represents a more selective approach than first-generation tau immunotherapies that targeted total tau:

• p-tau is pathologically relevant: Phosphorylated tau at specific sites (p-tau181, p-tau217, p-tau231) is specifically found in AD brain lesions, while total tau is elevated in various conditions[@ptau2024]
• Early detection marker: p-tau in CSF and plasma becomes abnormal early in AD pathogenesis, even before clinical symptoms
• Correlation with progression: p-tau levels correlate with cognitive decline and brain atrophy in AD

Active Immunotherapy Approach

Active immunotherapy (vaccination) differs from passive immunotherapy (monoclonal antibodies) in several key ways:

| Feature | Active (JNJ-64042056) | Passive (e.g., Lecanemab) |
|---------|----------------------|---------------------------|
| Administration | Subcutaneous/IM injection | IV infusion |
| Frequency | Less frequent (e.g., annually) | Frequent (e.g., biweekly) |
| Antibody production | Host generates antibodies | Exogenous antibodies delivered |
| Duration of effect | Potentially long-lasting | Requires continuous dosing |
| Immune response | Requires competent immune system | Direct delivery bypasses immunity |

Rationale for Targeting p-Tau

The selective targeting of p-tau provides several advantages[@tauvaccine2023]:

Scientific Background

Preclinical Alzheimer's Disease

Preclinical AD represents the earliest stage of Alzheimer's disease, characterized by[@alzheimers2023]:

• Amyloid positivity: Presence of amyloid plaques in the brain (detected via PET or CSF biomarkers)
• Evidence of tau pathology: Elevated p-tau in CSF or early tau PET signal
• Normal cognition: No clinically detectable cognitive impairment on standard tests
• Estimated duration: This stage may last 10-20 years before symptoms appear

Tau Biology in AD

The [tau protein](/proteins/tau), encoded by the [MAPT](/genes/mapt) gene, plays essential roles in neuronal function:

• Normal function: Stabilizes microtubules in axons, supporting axonal transport
• Pathological transformation: In AD, tau becomes hyperphosphorylated, leading to:
• Dissociation from microtubules
• Aggregation into neurofibrillary tangles (NFTs)
• Propagation between connected neurons
• Synaptic dysfunction and neuronal loss

Phosphorylation Sites

Key phosphorylation sites targeted by JNJ-64042056 include:

| Site | CSF Abnormality Timeline | Clinical Relevance |
|-----|------------------------|---------------------|
| p-tau181 | Earliest marker, rises ~20 years before onset | Strong predictor of progression |
| p-tau217 | Very early, correlates with amyloid | High specificity for AD |
| p-tau231 | Early marker, linked to tau PET | Associates with cognitive decline |

Study Design

This is a Phase 2, randomized, double-blind, placebo-controlled, parallel-group clinical trial with a long duration to assess preventive efficacy.

Key Design Features

• Population: Preclinical AD participants (amyloid positive, cognitively normal)
• Randomization: 1:1 active:placebo allocation
• Duration: Up to 206 weeks (~4 years) for efficacy assessment
• Primary endpoint: Change in Preclinical Alzheimer's Disease Cognitive Composite 5 (PACC-5)

Treatment Regimen

Participants receive:

• Active: JNJ-64042056 subcutaneous injections per protocol schedule
• Placebo: Matching placebo injections

Outcome Measures

Primary Endpoints

• PACC-5 Change: Change from baseline in Preclinical Alzheimer's Disease Cognitive Composite 5 at Week 206

Secondary Endpoints

• Clinical progression to MCI or dementia due to AD
• Brain amyloid PET change
• Tau PET change (regional)
• CSF biomarker changes (p-tau181, p-tau217, p-tau231, total tau)
• Plasma biomarker changes
• Safety and tolerability
• Immunogenicity (antibody titers)

Exploratory Endpoints

• Brain volume changes (MRI)
• Functional capacity measures
• Quality of life measures

Clinical Significance

Prevention Paradigm

This trial represents a critical step toward preventive neurology in AD[@aatc2024]:

Comparison to Other Approaches

| Trial | Approach | Target | Population | Stage |
|-------|----------|--------|------------|-------|
| JNJ-64042056 | Active immunotherapy | p-tau | Preclinical AD | Phase 2 |
| Leqembi (lecanemab) | Passive immunotherapy | Aβ aggregate | Early AD | Approved |
| Donanemab | Passive immunotherapy | N3pG Aβ | Early AD | Approved |
| Crenezumab | Passive immunotherapy | Aβ | Preclinical AD (API) | Phase 3 |

Regulatory Considerations

Preventive trials in preclinical populations face unique challenges:

• Long trial duration: Requires years of follow-up
• Large sample sizes: Need to detect subtle cognitive differences
• Ethical considerations: Treating asymptomatic individuals
• Biomarker qualification: Regulatory acceptance of surrogate endpoints

Safety Considerations

Active immunotherapy in healthy(appearing) individuals requires careful safety monitoring:

Common Considerations

• Injection site reactions: Typical with subcutaneous vaccines
• Systemic reactions: Fever, flu-like symptoms
• Autoimmune concerns: Theoretical risk of immune response against normal tau

Monitoring Plan

• Regular neurological examinations
• MRI to detect unexpected brain changes
• Cognitive monitoring for unexpected decline
• Immune response characterization

Related Pages

• [Phosphorylated Tau Biomarkers](/biomarkers/p-tau-181)
• [Phosphorylated Tau (p-tau217)](/biomarkers/p-tau-217)
• [Tau Immunotherapy](/therapeutics/tau-immunotherapy)
• [Preclinical Alzheimer's Disease](/diseases/preclinical-alzheimers)
• [Alzheimer's Disease Clinical Trials](/clinical-trials/alzheimers-disease-trials)
• [Janssen Neuroscience](/companies/janssen)
• [Tau Protein](/proteins/tau)
• [MAPT Gene](/genes/mapt)
• [Amyloid Cascade Hypothesis](/mechanisms/amyloid-cascade)

External Links

• [ClinicalTrials.gov: NCT06544616](https://clinicaltrials.gov/study/NCT06544616)
• [Janssen Pipeline](https://www.janssen.com/pipeline)
• [PubMed Search: JNJ-64042056](https://pubmed.ncbi.nlm.nih.gov/?term=JNJ-64042056)

References