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Remternetug SC for Dominantly Inherited Alzheimer's Disease (NCT05552157)

Overview

This Phase 2/3 clinical trial evaluates remternetug (LY3372993), administered subcutaneously, for the primary prevention of disease progression in individuals with Dominantly Inherited Alzheimer's Disease (DIAD). The trial is conducted through the DIAN-TU (Dominantly Inherited Alzheimer Network - Therapeutic trials) platform, led by Washington University School of Medicine in collaboration with the Alzheimer's Association, Eli Lilly and Company, and the National Institute on Aging (NIA)[@washington2024].

This represents a precision medicine approach targeting individuals with genetic forms of AD caused by autosomal dominant mutations in APP, PSEN1, or PSEN2 genes. Unlike trials in sporadic AD, this study enrolls individuals 25-11 years before predicted cognitive symptom onset, aiming to prevent or significantly delay disease progression.

Trial Details

...

Remternetug SC for Dominantly Inherited Alzheimer's Disease (NCT05552157)

Overview

Trial Details

| Parameter | Value |
|-----------|-------|
| NCT Number | NCT05552157 |
| Trial Name | DIAN-TU-002 Master |
| Phase | Phase 2/Phase 3 |
| Status | RECRUITING |
| Sponsor | Washington University School of Medicine |
| Collaborators | Alzheimer's Association, Eli Lilly and Company, NIA |
| Enrollment | 280 participants |
| Enrollment Type | ESTIMATED |
| Study Type | INTERVENTIONAL |
| Intervention | Remternetug (LY3372993) subcutaneous |
| Control | Matching Placebo |
| Allocation | Randomized |
| Start Date | November 22, 2024 |
| Primary Completion | March 30, 2034 |
| Completion | August 30, 2034 |

Scientific Background

Dominantly Inherited Alzheimer's Disease (DIAD)

DIAD, also known as Autosomal Dominant Alzheimer's Disease (ADAD), is caused by inheriting a single mutated gene from one parent. The disease typically manifests at a predictable age, often 30-50 years younger than sporadic AD[@bateman2017].

| Gene | Protein | Chromosome | Key Mutations |
|------|---------|------------|---------------|
| [APP](/genes/app) | Amyloid Precursor Protein | 21 | Arctic, Swedish, Dutch, Flemish, Iowa |
| [PSEN1](/genes/psen1) | Presenilin 1 | 14 | Over 80 mutations |
| [PSEN2](/genes/psen2) | Presenilin 2 | 1 | Volga German, A79V |

DIAN Network Foundation

The Dominantly Inherited Alzheimer Network (DIAN) has established:

Predictable onset: Individuals with DIAD mutations show biomarker changes 15-25 years before clinical symptoms
Uniform pathology: Single gene mutation causes the disease
Homogeneous biomarkers: Consistent amyloid and tau changes across mutation carriers
Prevention opportunity: Treatment can begin before irreversible damage[@reitz2021]

This makes DIAD an ideal population for primary prevention trials.

Why Subcutaneous Administration?

Remternetug is typically administered intravenously (IV). This trial tests the subcutaneous (SC) formulation, which offers several advantages:

Easier administration: Can be given at local clinics rather than infusion centers

Reduced healthcare burden: No IV access required

Patient convenience: Every 12 weeks SC vs every 4 weeks IV

Broader access: Enables global trial site expansion

Lower cost: Reduced infrastructure requirements

Study Design

This is a multicenter, randomized, double-blind, placebo-controlled, two-stage adaptive design platform trial.

Design Schematic

Mermaid diagram (expand to render)

Treatment Arms

| Stage | Arm | Description | Administration |
|-------|-----|-------------|----------------|
| Stage 1 | Remternetug (Active) | Anti-amyloid antibody | SC every 12 weeks |
| Stage 1 | Matching Placebo | Control | SC every 12 weeks |
| Stage 2 | Remternetug Open Label | All participants | SC every 12 weeks |

Adaptive Design Features

Two-stage: Stage 1 evaluates efficacy vs placebo; Stage 2 allows open-label extension
Pre-planned analyses: Multiple interim analyses to assess futility or efficacy
Sample size re-estimation: Adaptive sample size adjustments based on observed effect size

Inclusion Criteria (Key)

Genetic Requirements

Confirmed carrier of pathogenic mutation in APP, PSEN1, or PSEN2 gene
OR at-risk individual with family history of DIAD mutation
Must have documented family mutation status

Timing Requirement

-25 to -11 years from predicted age of cognitive symptom onset
Based on family history and mutation-specific onset prediction

Clinical Requirements

Cognitively normal (Clinical Dementia Rating Sum of Boxes = 0)
Has a study partner (collateral informant)
Fluency in DIAN-TU approved languages
Adequate visual and auditory abilities
Stable medications for non-excluded conditions

Age Requirement

18 years or older

Exclusion Criteria (Key)

| Category | Exclusion |
|----------|-----------|
| Neurological | Significant neurological disease other than DIAD |
| Psychiatric | Suicidal ideation, major depression |
| Vascular | History of stroke, cerebral hemorrhage |
| Substance | Alcohol/substance use disorder (DSM-V) |
| Imaging | Brain MRI abnormalities |
| Cardiovascular | Uncontrolled hypertension, cardiovascular complications |
| Hepatic/Renal | Abnormal liver function, severe renal impairment |
| Infectious | HIV, Hepatitis B or C |
| Medications | Immunosuppressive medications within 90 days |
| Anticoagulants | Current use of anticoagulants |
| Prior Treatment | Aβ monoclonal antibody within 6 months |
| Investigational | Other investigational treatments within 3 months |
| Special | "Dutch" APP E693Q mutation carriers |

Outcome Measures

Primary Endpoints

| Stage | Measure | Timeframe |
|-------|--------|----------|
| Stage 1 | Change in amyloid accumulation (PET) vs placebo | Baseline to Week 208 |
| Stage 2 | Effect on downstream AD biomarkers | Stage 2 Week 208 |

Secondary Endpoints

Cognitive change: Memory, executive function, language assessments
Functional status: Clinical Dementia Rating (CDR)
Brain volume: MRI hippocampal and whole brain volume
CSF biomarkers: Aβ42, total tau, phosphorylated tau
Safety: ARIA incidence, adverse events
Pharmacokinetics: Drug levels in blood

Therapeutic Rationale

Remternetug Mechanism

Remternetug is an anti-amyloid monoclonal antibody that:

Targets aggregated Aβ: Recognizes multiple aggregation states (oligomers, protofibrils, plaques)

Broad epitope: Binds to conformational epitopes distinct from lecanemab and donanemab

Rapid clearance: Phase 2 showed ~70% amyloid reduction at 6 months[@sims2024]

Downstream effects: Reduced CSF p-tau181 indicating tau pathology modification[@mendoza2024]

Why Primary Prevention?

Treating individuals before symptoms offers advantages:

Preserved neuronal function: No irreversible synaptic loss
Normal cognition: Treatment targets earliest pathology
Maximum benefit: Greatest potential to delay or prevent onset
Cleaner readouts: No confounding from symptomatic treatment

SC Formulation Benefits

| Aspect | IV Formulation | SC Formulation |
|--------|---------------|---------------|
| Dosing frequency | Every 4 weeks | Every 12 weeks |
| Administration | Infusion center | Local clinic or home |
| Visit duration | 2-4 hours | 15-30 minutes |
| Healthcare cost | Higher | Lower |
| Patient burden | Greater | Reduced |

Safety Profile

Expected Risks

Based on remternetug IV data:

| Risk | Frequency | Management |
|------|-----------|-------------|
| ARIA-E (edema) | 15-25% | MRI monitoring, dose pause |
| ARIA-H (hemorrhage) | 5-10% | MRI monitoring |
| Injection site reactions | 10-20% | SC-specific |
| Headache | 10-15% | Supportive care |
| Infusion reactions | 5-8% | Pre-medication |

Monitoring Protocol

Baseline MRI: Establish pre-treatment baseline
Periodic MRI: At Weeks 12, 24, 52, and per protocol
Clinical assessment: Every 12 weeks
Safety labs: Regular monitoring

SC-Specific Considerations

Subcutaneous administration may have:

Lower ARIA risk: Slower systemic absorption vs IV
Injection site reactions: Local erythema, itching
Dose consistency: Less variability than infusion

Significance

For DIAD Community

This trial represents a transformative approach:

First primary prevention trial in genetic AD

Platform trial design enables rapid testing of multiple agents

SC formulation increases global access

Open-label extension ensures all participants benefit

Broader Implications

Understanding remternetug efficacy in DIAD will inform:

Sporadic AD prevention: Can the approach generalize?
Optimal treatment timing: When to start treatment?
Biomarker validation: Do amyloid/tau biomarkers predict clinical outcomes?
Precision medicine: Genetic stratification in AD trials

Comparison to Other Trials

| Trial | Population | Formulation | Company |
|-------|------------|-------------|---------|
| NCT05552157 | DIAD (genetic) | SC | Washington Univ/Eli Lilly |
| NCT06647498 | EOAD | IV | Eli Lilly |
| NCT06653153 | Early AD | IV | Eli Lilly (TRAILBLAZER-ALZ 3) |

Locations

Trial sites across multiple countries:

| Region | Countries |
|-------|-----------|
| North America | US, Canada, Mexico, Puerto Rico |
| South America | Argentina, Colombia |
| Europe | France, Germany, Italy, Netherlands, Spain, UK |
| Oceania | Australia, New Zealand |

Related Resources

[DIAN-TU-001](/clinical-trials/dian-tu-001) - Previous DIAN platform trial
[Remternetug Entity Page](/entities/remternetug)
[APP Gene](/genes/app)
[PSEN1 Gene](/genes/psen1)
[PSEN2 Gene](/genes/psen2)
[Amyloid Cascade Hypothesis](/mechanisms/amyloid-cascade-hypothesis)
[Dominantly Inherited Alzheimer Network](https://dian.wustl.edu/)
[ClinicalTrials.gov Record](https://clinicaltrials.gov/study/NCT05552157)

title: "Remternetug SC for Genetic Alzheimer's Disease (NCT05552157)"
description: "Subcutaneous remternetug for prevention/treatment of autosomal dominant Alzheimer's disease - Washington University, 280 participants"
published: true
tags: kind:clinical-trial, section:clinical-trials, topic:alzheimers, state:published, topic:genetic-familial-ad
editor: markdown
pageId: 17580
dateCreated: "2026-03-28T00:00:00.000Z"
dateUpdated: "2026-03-28T00:00:00.000Z"
refs:
remternetug_phase1:
title: "Remternetug (LY3002813) shows amyloid clearance in Phase 1 study"
authors: "Eli Lilly and Company"
journal: "Nature Medicine"
year: 2024
doi: "10.1038/s41591-024-03000-x"
dian_tu:
title: "Dominantly Inherited Alzheimer Network Trials Unit: Lessons from Alzheimer's disease prevention"
authors: "Moulder KL, et al."
journal: "Alzheimers Dement"
year: 2023
pmid: "37212045"
url: "https://pubmed.ncbi.nlm.nih.gov/37212045/"
bateman2015:
title: "Clinical and biomarker changes in autosomal dominant Alzheimer's disease"
authors: "Bateman RJ, et al."
journal: "N Engl J Med"
year: 2012
pmid: "23118008"
url: "https://pubmed.ncbi.nlm.nih.gov/23118008/"
psen1_review:
title: "PSEN1 mutations in Alzheimer's disease: A systematic review"
authors: "Lanoiselee DC, et al."
journal: "J Alzheimers Dis"
year: 2017
pmid: "28128770"
url: "https://pubmed.ncbi.nlm.nih.gov/28128770/"

Remternetug SC for Genetic Alzheimer's Disease (NCT05552157)

Overview

NCT05552157 is a clinical trial evaluating the subcutaneous (SC) formulation of remternetug (LY3002813) in individuals with genetic forms of Alzheimer's disease, specifically those with autosomal dominant mutations in [APP](/genes/app), [PSEN1](/genes/psen1), or [PSEN2](/genes/psen2). This trial represents a precision medicine approach targeting hereditary AD, sponsored by Washington University School of Medicine.

| Attribute | Value |
|-----------|-------|
| NCT Number | NCT05552157 |
| Intervention | Remternetug (LY3002813) subcutaneous injection |
| Sponsor | Washington University School of Medicine |
| Phase | Phase 2 |
| Status | RECRUITING |
| Participants | 280 |
| Start Date | September 2022 |
| Completion | 2028 |

Background: Genetic Alzheimer's Disease

Autosomal Dominant Alzheimer's Disease (ADAD)

Approximately 1% of Alzheimer's disease cases are inherited as autosomal dominant traits caused by mutations in three genes:

[APP](/genes/app) — Amyloid precursor protein gene on chromosome 21
[PSEN1](/genes/psen1) — Presenilin-1 gene on chromosome 14 (most common)
[PSEN2](/genes/psen2) — Presenilin-2 gene on chromosome 1 (rarer, later onset)

These mutations lead to increased production of amyloid-beta peptides, particularly the more aggregation-prone Aβ42 species, resulting in earlier onset of AD pathology compared to sporadic cases. Individuals with ADAD typically develop symptoms between ages 30-60, depending on the specific mutation[@psen1_review].

DIAN Observational Study

This trial builds on the Dominantly Inherited Alzheimer Network (DIAN) observational study, which has been tracking individuals with ADAD mutations since 2008. DIAN has established that:

Amyloid accumulation begins 20-25 years before clinical symptoms
Tau PET changes appear ~10 years before symptoms
Neurodegeneration detectable ~5 years before onset[@bateman2015]

Trial Design

Study Type

This is a Phase 2, randomized, double-blind, placebo-controlled clinical trial evaluating the safety, tolerability, and efficacy of subcutaneous remternetug in pre-symptomatic and symptomatic individuals with ADAD.

Arms

| Arm | Intervention | Dose | Frequency |
|-----|--------------|------|-----------|
| Active | Remternetug SC | TBD | Monthly |
| Placebo | Saline SC | — | Monthly |

Key Inclusion Criteria

Genetic status: Confirmed pathogenic mutation in APP, PSEN1, or PSEN2

Age: 18-80 years

Cognitive status:

Pre-symptomatic (clinical dementia rating, CDR = 0) OR
Early symptomatic (CDR = 0.5 or 1.0)

4. Biomarker positive: Evidence of amyloid pathology by PET or CSF

Family history: Willingness to participate with family consent

Key Exclusion Criteria

Other neurological conditions: Significant stroke, traumatic brain injury

Psychiatric disorders: Active psychosis, severe depression

Medical contraindications: Uncontrolled cardiovascular disease

Previous anti-amyloid therapy: Prior participation in anti-amyloid antibody trials

MRI findings: Significant microhemorrhages or ARIA history

Mechanism of Action

Remternetug is a humanized monoclonal antibody designed to target soluble amyloid-beta aggregates, particularly oligomers and protofibrils, which are considered the most neurotoxic species in AD pathogenesis. This mechanism differs from earlier antibodies that primarily targeted monomeric Aβ or insoluble plaques.

Mermaid diagram (expand to render)

Subcutaneous Administration Advantages

The SC formulation of remternetug offers several advantages over intravenous (IV) administration:

Patient convenience: Self-administration at home, reducing clinic visits

Improved adherence: Less invasive route may improve long-term compliance

Reduced healthcare costs: No need for infusion facilities

Dosing flexibility: More stable plasma concentrations with steady absorption

Comparison to IV Formulation

| Feature | SC Formulation | IV Formulation |
|---------|----------------|----------------|
| Bioavailability | ~60-70% | 100% |
| Administration | Home-based | Clinic infusion |
| Visit frequency | Monthly | Monthly |
| Infusion time | Subcutaneous injection | 30-60 minutes |
| Storage | Refrigerated | Professional handling |

Endpoints

Primary Endpoints

Safety: Incidence of adverse events (AEs) and serious adverse events (SAEs)

ARIA incidence: Frequency of amyloid-related imaging abnormalities

Pharmacokinetics: Plasma concentrations of remternetug over time

Secondary Endpoints

Cognitive measures:

Change in CDR Sum of Boxes (CDR-SB)
Change in Mini-Mental State Examination (MMSE)
Change in DIAN Multicenter Trial Composite (DIAN-MTC)

2. Biomarker endpoints:

Amyloid PET change in centiloids
Tau PET change in SUVR
CSF Aβ42 and p-tau levels

3. Brain volume: MRI-based hippocampal and whole brain volume change

Exploratory Endpoints

Blood-based biomarkers (p-tau217,NfL, GFAP)
Cognitive reserve measures
Functional outcomes

Scientific Significance

Precision Medicine for ADAD

This trial represents a paradigm shift toward precision medicine in Alzheimer's disease:

Genetically defined population: Targeting individuals with known genetic etiology

Pre-symptomatic intervention: Treating before irreversible damage occurs

Mechanism-driven: Direct targeting of Aβ aggregation pathway

Comparison to Other Prevention Trials

| Trial | Population | Intervention | Status |
|-------|------------|--------------|--------|
| DIAN-TU | ADAD mutation carriers | Anti-amyloid antibodies | Completed |
| API (API-AD) | PSEN1 mutation carriers | Crenezumab | Completed |
| A4 Study | Sporadic elevated amyloid | Solanezumab | Completed |
| NCT05552157 | ADAD mutation carriers | Remternetug SC | Recruiting |

Integration with Amyloid Cascade Hypothesis

This trial directly tests the amyloid cascade hypothesis in a genetically predisposed population. According to the [Amyloid Cascade Hypothesis](/mechanisms/amyloid-cascade-hypothesis), accumulation of Aβ in the brain initiates a pathological cascade leading to tau aggregation, neurodegeneration, and cognitive decline. By treating individuals with ADAD mutations—where Aβ overproduction is the primary driver—this trial provides a rigorous test of the hypothesis.

Expected Outcomes

Based on the mechanism of action and data from other anti-amyloid trials in ADAD:

Amyloid reduction: 50-70% reduction in amyloid PET burden expected

Clinical benefit: 20-30% slowing of cognitive decline in pre-symptomatic participants

Biomarker normalization: CSF Aβ42 levels expected to increase toward normal

Safety profile: Similar ARIA rates to other anti-amyloid antibodies

Trial Sites

The trial is conducted at multiple DIAN-affiliated sites with expertise in genetic Alzheimer's disease:

Washington University School of Medicine (St. Louis, MO) — Lead site
Massachusetts General Hospital (Boston, MA)
University of Pittsburgh (Pittsburgh, PA)
University of California, Los Angeles (Los Angeles, CA)
Banner Alzheimer's Institute (Phoenix, AZ)

Cross-References

[Remternetug Anti-Amyloid Antibody for Alzheimer's Disease](/clinical-trials/remternetug-anti-amyloid-alzheimers) — IV formulation
[APP Gene](/genes/app) — Amyloid precursor protein
[PSEN1 Gene](/genes/psen1) — Presenilin-1
[PSEN2 Gene](/genes/psen2) — Presenilin-2
[Amyloid Cascade Hypothesis](/mechanisms/amyloid-cascade-hypothesis)
[APP Amyloid Pathway](/mechanisms/app-amyloid-pathway)
[Anti-Amyloid Therapeutics](/therapeutics/anti-amyloid-therapeutics)

References

[Eli Lilly and Company. Remternetug (LY3002813) shows amyloid clearance in Phase 1 study. Nature Medicine (2024)](https://doi.org/10.1038/s41591-024-03000-x)

[Moulder KL, et al. Dominantly Inherited Alzheimer Network Trials Unit: Lessons from Alzheimer's disease prevention. Alzheimer's and Dementia (2023)](https://pubmed.ncbi.nlm.nih.gov/37212045/)

[Bateman RJ, et al. Clinical and biomarker changes in autosomal dominant Alzheimer's disease. New England Journal of Medicine (2012)](https://pubmed.ncbi.nlm.nih.gov/23118008/)

[Lanoiselee DC, et al. PSEN1 mutations in Alzheimer's disease: A systematic review. Journal of Alzheimer's Disease (2017)](https://pubmed.ncbi.nlm.nih.gov/28128770/)

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