Trontinemab (RO7126209) Phase 3 Trial — TRONTIER 2 (NCT07170150)

Trontinemab NCT07170150

Overview

Trontinemab (RO7126209) Phase 3 Trial — TRONTIER 2 (NCT07170150) is a pivotal Phase 3 clinical trial evaluating trontinemab, an innovative anti-tau antibody with enhanced brain penetration, in patients with early symptomatic Alzheimer's disease. This trial represents a significant advancement in tau-directed immunotherapy for Alzheimer's disease, combining a novel mechanism of action with an advanced delivery technology designed to overcome one of the greatest challenges in CNS drug development: effective antibody delivery across the blood-brain barrier["@clinicaltrialsgov"][@roche].

Trial Overview

| Field | Value |
|-------|-------|
| NCT ID | [NCT07170150](https://clinicaltrials.gov/NCT07170150) |
| Phase | Phase 3 |
| Status | Recruiting |
| Sponsor | Hoffmann-La Roche |
| Acronym | TRONTIER 2 |
| Start Date | November 12, 2025 |
| Primary Completion | June 7, 2028 |
| Enrollment | 800 participants |
| Study Design | Randomized, double-blind, placebo-controlled |
| Treatment Duration | 72 weeks (18 months) |
| Follow-up | 28 weeks post-treatment |

Study Design

Trontinemab NCT07170150

Overview

Trontinemab (RO7126209) Phase 3 Trial — TRONTIER 2 (NCT07170150) is a pivotal Phase 3 clinical trial evaluating trontinemab, an innovative anti-tau antibody with enhanced brain penetration, in patients with early symptomatic Alzheimer's disease. This trial represents a significant advancement in tau-directed immunotherapy for Alzheimer's disease, combining a novel mechanism of action with an advanced delivery technology designed to overcome one of the greatest challenges in CNS drug development: effective antibody delivery across the blood-brain barrier["@clinicaltrialsgov"][@roche].

Trial Overview

| Field | Value |
|-------|-------|
| NCT ID | [NCT07170150](https://clinicaltrials.gov/NCT07170150) |
| Phase | Phase 3 |
| Status | Recruiting |
| Sponsor | Hoffmann-La Roche |
| Acronym | TRONTIER 2 |
| Start Date | November 12, 2025 |
| Primary Completion | June 7, 2028 |
| Enrollment | 800 participants |
| Study Design | Randomized, double-blind, placebo-controlled |
| Treatment Duration | 72 weeks (18 months) |
| Follow-up | 28 weeks post-treatment |

Study Design

TRONTIER 2 is a Phase III, multicenter, randomized, double-blind, placebo-controlled, parallel-group efficacy and safety study of trontinemab in participants with early symptomatic Alzheimer's disease (MCI to mild dementia due to AD)[@clinicaltrialsgov]. The trial employs a sophisticated design with multiple arms and extensive biomarker substudies.

Arms

| Arm | Type | Description | Dose |
|-----|------|-------------|------|
| Trontinemab Low Dose | Experimental | IV infusion of trontinemab | TBD |
| Trontinemab High Dose | Experimental | IV infusion of trontinemab | TBD |
| Placebo | Placebo Comparator | IV infusion of placebo | N/A |

Randomization

• Ratio: 1:1:1 (low dose : high dose : placebo)
• Stratification: By age, baseline cognitive status, and ApoE status
• Blinding: Double-blind maintained through all treatment and follow-up periods

Key Eligibility

Inclusion Criteria:

• Condition: Early symptomatic Alzheimer's disease (MCI to mild dementia due to AD)
• Age: 50-85 years
• MMSE: 20-28 (inclusive)
• Clinical Dementia Rating (CDR): 0.5 or 1.0
• Amyloid positivity: Confirmed by PET or CSF biomarkers
• Brain MRI: Consistent with AD, no significant vascular pathology
• Stable on background AD therapy (if applicable)

• Significant psychiatric illness
• Active neurological disease other than AD
• History of stroke or significant vascular disease
• Contraindications to MRI
• Prior anti-tau immunotherapy

Mechanism of Action

Anti-Tau Antibody

Trontinemab (RO7126209) is an anti-tau antibody designed to target pathological tau protein in the brain[@tau_immunotherapy]. Tau protein is a microtubule-associated protein that, in Alzheimer's disease, becomes hyperphosphorylated, aggregates into neurofibrillary tangles (NFTs), and propagates throughout the brain in a predictable pattern that closely correlates with cognitive decline.

Tau Pathology in AD

The tau protein undergoes several pathological modifications in Alzheimer's disease:

The "Braak staging" system describes the progression of tau pathology through the brain in a hierarchical manner, beginning in the entorhinal cortex and spreading to the hippocampus, limbic structures, and eventually throughout the neocortex.

Brain Shuttle Technology

The key innovation of trontinemab is the Brain Shuttle technology, which enhances delivery of the antibody across the blood-brain barrier (BBB)[@brain_shuttle_technology]. This approach aims to overcome the traditional challenge of limited CNS penetration for large molecule therapeutics.

How the Brain Shuttle Works

Advantages

• Increased brain exposure: Up to 10-20x higher brain concentrations compared to conventional antibodies
• Reduced peripheral exposure: Lower doses may achieve therapeutic brain levels
• Improved target engagement: Better occupancy of tau targets in the brain
• Potential for lower dosing: Reduced risk of peripheral side effects

Preclinical Data

In preclinical models, the Brain Shuttle technology demonstrated[@brain_shuttle_technology]:

• Enhanced brain uptake in non-human primates
• Reduced plaque-bound antibody in periphery
• Improved distribution throughout brain parenchyma
• Maintained target engagement in tau pathology models

Phase 1 Results

The first-in-human study of trontinemab showed promising results[@trontinemab_phase1]:

• Safety: Generally well-tolerated with no dose-limiting toxicities
• Pharmacokinetics: Extended half-life supporting less frequent dosing
• Target engagement: Dose-dependent reduction in CSF tau species
• Biomarker signals: Encouraging effects on neurodegeneration markers
• ARIA: Low rates of amyloid-related imaging abnormalities (ARIA)

Outcomes

Primary Outcome

• Change from baseline to Week 72 in Clinical Dementia Rating, Sum of Boxes (CDR-SB)

Secondary Outcomes

Cognitive Measures

• ADAS-Cog-13: Alzheimer's Disease Assessment Scale - Cognitive subscale (13-item version)
• MMSE: Mini-Mental State Examination
• NCTR-ERB: Neuropsychological Test Battery with Emotional Recognition

Functional Measures

• ADCS-ADL: Alzheimer's Disease Cooperative Study - Activities of Daily Living
• iADRS: Integrated Alzheimer's Disease Rating Scale (composite of cognitive and functional)

Biomarker Outcomes

• Brain amyloid load: Amyloid PET (Centiloid scale)
• Brain tau load: Tau PET (subset of participants)
• CSF biomarkers:
• Phosphorylated tau (p-tau181)
• Total tau
• Neurogranin (synaptic marker)
• Aβ42/40 ratio
• Blood biomarkers:
• Plasma p-tau217
• GFAP (Glial Fibrillary Acidic Protein)
• NfL (Neurofilament Light Chain)

Safety Outcomes

• ARIA-E/E: Amyloid-related imaging abnormalities - edema/effusion
• ARIA-H: Amyloid-related imaging abnormalities - hemorrhage
• Infusion reactions: Rate and severity
• Anti-drug antibodies: Immunogenicity assessment
• Adverse events: Comprehensive safety monitoring

Exploratory Outcomes

• Brain volume: MRI volumetric measures (hippocampus, ventricles)
• Connectivity: Resting-state fMRI
• Digital biomarkers: Smartphone-based cognitive assessments
• Pharmacogenomics: ApoE genotype effects on response

Clinical Significance

Positioning in AD Therapeutic Landscape

Trontinemab represents a next-generation approach in the AD therapeutic pipeline:

Challenges in Tau Immunotherapy

Tau immunotherapy faces several challenges that trontinemab's design addresses:

• BBB penetration: Brain Shuttle technology specifically addresses this
• Target specificity: Trontinemab targets pathological tau specifically
• Off-target effects: Engineered Fc reduces peripheral binding
• Immunogenicity: Humanized antibody design minimizes immune response

Comparison with Other Anti-Tau Approaches

| Approach | Company | Stage | Mechanism |
|-------------|------------|-----------|---------------|
| Trontinemab (RO7126209) | Roche | Phase 3 | Anti-tau antibody with Brain Shuttle |
| Semorinemab | Genentech | Phase 2 | Anti-tau antibody |
| Tilavonemab | AbbVie | Phase 2 | Anti-tau antibody |
| JNJ-63733657 | Janssen | Phase 1 | Anti-tau antibody |
| BIIB080 | Biogen | Phase 1 | Anti-tau ASO |

Trial Locations

The trial is being conducted at multiple sites globally, including in the United States, United Kingdom, Germany, France, Spain, Italy, Japan, South Korea, Australia, and Canada. For current site information, visit [ClinicalTrials.gov](https://clinicaltrials.gov/NCT07170150).

United States Sites

International Sites

• United Kingdom: Multiple NHS trusts and private hospitals
• Europe: Sites in Germany (Charité, etc.), France, Spain, Italy
• Asia-Pacific: Japan, South Korea, Australia

Future Directions

Long-term Follow-up

• Extension studies: Planned to assess long-term safety and efficacy
• Open-label phases: Potential for participants to receive active treatment

Combination Approaches

• Anti-amyloid combination: Rationale for combining with approved anti-amyloid antibodies
• Small molecule combinations: Potential with symptomatic treatments

Biomarker Development

• Patient selection: Refinement of biomarker-based patient selection
• Response prediction: Identification of predictors of treatment response
• Monitoring: Development of real-time biomarker monitoring approaches

Related Pages

• [Alzheimer's Disease](/diseases/alzheimers-disease)
• [Tau Pathology](/mechanisms/tau-pathology)
• [Anti-Tau Therapies](/therapeutics/anti-tau-therapies)
• [Blood-Brain Barrier Drug Delivery](/technologies/brain-shuttle-technology)
• [Clinical Trials Index](/clinical-trials)
• [Amyloid Immunotherapy](/therapeutics/amyloid-immunotherapy)
• [Tau PET Imaging](/diagnostics/tau-pet-imaging)

External Links

• [ClinicalTrials.gov - NCT07170150](https://clinicaltrials.gov/NCT07170150)
• [Roche Research Pipeline](https://www.roche.com/research/pipeline)
• [Roche CNS Innovation](https://www.roche.com/)
• [Alzheimer's Association](https://www.alz.org/)
• [ALZforum Trial Tracker](https://www.alzforum.org/)

References