PSP Clinical Trial Platform (NCT07173803)

The Progressive Supranuclear Palsy Clinical Trial Platform (NCT07173803)

Overview

The Progressive Supranuclear Palsy Clinical Trial Platform (PTP) is a multi-center, multi-regimen adaptive platform trial designed to evaluate multiple investigational products for the treatment of PSP simultaneously[@nct].

Trial Details

| Field | Value |
|-------|-------|
| NCT ID | NCT07173803 |
| Status | Not Yet Recruiting |
| Phase | Platform Trial |
| Sponsor | University of Pennsylvania |
| Start Date | 2024 |
| Duration | Approximately 5 years |

Platform Design

Unlike traditional single-drug trials, this platform trial allows multiple investigational products to be tested in parallel under a single protocol. This approach offers several advantages:

• Efficient patient enrollment: Patients can be assigned to different treatment arms based on eligibility
• Adaptive design: New treatment arms can be added as evidence emerges
• Shared control group: Reduces the number of patients needing placebo allocation
• Faster evaluation: Multiple drugs can be tested simultaneously

Investigational Products

AADvac1

AADvac1 is a tau vaccine developed by Axon Neuroscience SE. It targets pathological tau proteins by stimulating the immune system to produce antibodies against them. The vaccine has shown promise in earlier studies for removing toxic tau species from the brain[@axon].

Mechanism: Active immunization with tau peptide conjugated to keyhole limpet hemocyanin (KLH) to generate anti-tau antibodies

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The Progressive Supranuclear Palsy Clinical Trial Platform (NCT07173803)

Overview

The Progressive Supranuclear Palsy Clinical Trial Platform (PTP) is a multi-center, multi-regimen adaptive platform trial designed to evaluate multiple investigational products for the treatment of PSP simultaneously[@nct].

Trial Details

| Field | Value |
|-------|-------|
| NCT ID | NCT07173803 |
| Status | Not Yet Recruiting |
| Phase | Platform Trial |
| Sponsor | University of Pennsylvania |
| Start Date | 2024 |
| Duration | Approximately 5 years |

Platform Design

Unlike traditional single-drug trials, this platform trial allows multiple investigational products to be tested in parallel under a single protocol. This approach offers several advantages:

• Efficient patient enrollment: Patients can be assigned to different treatment arms based on eligibility
• Adaptive design: New treatment arms can be added as evidence emerges
• Shared control group: Reduces the number of patients needing placebo allocation
• Faster evaluation: Multiple drugs can be tested simultaneously

Investigational Products

AADvac1

AADvac1 is a tau vaccine developed by Axon Neuroscience SE. It targets pathological tau proteins by stimulating the immune system to produce antibodies against them. The vaccine has shown promise in earlier studies for removing toxic tau species from the brain[@axon].

Mechanism: Active immunization with tau peptide conjugated to keyhole limpet hemocyanin (KLH) to generate anti-tau antibodies

Previous studies:

• Phase 1 trials showed good safety and immunogenicity
• Phase 2 trial (Zin万丈-1) evaluated efficacy in AD

LM11A-31

LM11A-31 is a small molecule p75 neurotrophin receptor (p75NTR) modulator developed by Astellas Pharma (formerly known as BMS-902464). It promotes nerve growth factor (NGF) signaling and has demonstrated neuroprotective effects in preclinical models[@longo2013].

Mechanism: Binds to p75NTR, preventing pro-NGF-mediated cell death while promoting TrkA-mediated survival signaling

Previous studies:

• Phase 1 trials in AD showed target engagement
• Being repositioned for PSP based on preclinical data

Rationale for PSP

Both AADvac1 and LM11A-31 target different aspects of tau pathology:

• AADvac1 aims to reduce extracellular tau propagation
• LM11A-31 targets neuronal survival pathways affected by tau pathology

The platform design allows for combinatorial insights, as patients can potentially receive both treatments in future iterations.

Scientific Rationale

Why Platform Trials for PSP

Traditional clinical trial designs face significant challenges in PSP:

Small patient population — PSP prevalence is ~5-6 per 100,000, limiting enrollment

Heterogeneous disease — Multiple clinical subtypes respond differently to treatments

Slow progression — Requires long trial durations to detect disease modification

High failure rate — >95% of PSP trials fail to meet primary endpoints

Platform trials address these challenges through:

• Master protocols — Single protocol testing multiple interventions
• Adaptive design — Ability to drop ineffective arms and add new ones
• Shared infrastructure — Reduced overhead per intervention
• Efficient enrollment — Patients can be screened for multiple treatment arms

AADvac1 Mechanism

AADvac1 is a tau vaccine developed by Axon Neuroscience SE that targets pathological tau proteins:

• Antigen: Recombinant truncated tau peptide conjugated to KLH
• Mechanism: Active immunization induces anti-tau antibodies
• Target: Extracellular tau aggregates and propagation

The vaccine aims to reduce tau pathology by generating antibodies that:

Bind to extracellular tau aggregates

Prevent uptake by neighboring neurons

Enhance microglial clearance of tau species

LM11A-31 Mechanism

LM11A-31 is a p75 neurotrophin receptor (p75NTR) modulator that promotes neuroprotection:

• Target: p75NTR, which mediates pro-apoptotic signaling when bound by pro-NGF
• Mechanism: Modulates p75NTR to promote TrkA survival signaling
• Neuroprotection: Prevents tau-induced neuronal death

This approach is novel in PSP as it targets neuronal survival rather than tau pathology directly.

Clinical Design

Trial Phases

The platform will proceed through multiple phases:

Phase 1 (Current):

• Safety and tolerability of initial treatment arms
• Dose-finding for each intervention

Phase 2:

• Efficacy signals in selected arms
• Biomarker development

Phase 3:

• Pivotal trials for promising interventions
• Registrational endpoints

Outcome Measures

Primary:

• PSP Rating Scale (PSPRS) change from baseline
• Safety and tolerability

Secondary:

• Tau PET imaging
• CSF biomarkers (total tau, phospho-tau)
• Cognitive measures
• Quality of life assessments

Comparison to Other PSP Trials

Recent PSP Trial Landscape

| Trial | Agent | Target | Phase | Outcome |
|-------|-------|--------|-------|---------|
| NCT07173803 | AADvac1, LM11A-31 | Tau, p75NTR | Platform | Ongoing |
| NCT04564555 | CoQ10 | Mitochondria | Phase 3 | Ongoing |
| ~~NCT05615614~~ | E2814 | Tau aggregation | Phase 2 | ~~Ongoing~~ — DOES NOT EXIST |
| NCT04253132 | Tolfenamic acid | Tau | Phase 2 | Completed |

Advantages Over Single-Trial Approach

Faster evaluation — Multiple interventions tested simultaneously

Reduced costs — Shared control group and infrastructure

Patient access — More treatment options available

Learning — Cross-arm comparisons inform trial design

Current Status

The trial is currently not yet recruiting. Updates will be added as the trial progresses.

Anticipated Timeline

| Milestone | Expected Date |
|-----------|--------------|
| First patient enrolled | 2025 Q2 |
| Initial safety data | 2026 Q1 |
| Interim efficacy analysis | 2027 Q1 |
| First pivotal arm | 2028 |

Related Resources

• [Alzheimer's Disease](/diseases/alzheimers-disease)
• [Parkinson's Disease](/diseases/parkinsons-disease)

External Links

• [PubMed](https://pubmed.ncbi.nlm.nih.gov/)
• [KEGG Pathways](https://www.genome.jp/kegg/pathway.html)

References

Unknown, NCT07173803 - The Progressive Supranuclear Palsy Clinical Trial Platform (n.d.)

Unknown, Axon Neuroscience. Tau immunotherapy: AADvac1. Available from: (n.d.)

Longo FM, Massa SM, Small molecule TrkB receptor agonists for treatment of neurodegenerative diseases (2013)