Syntenin-1 Exosome Biogenesis Modulation Therapy for Neurodegeneration

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Syntenin-1 Exosome Biogenesis Modulation Therapy for Neurodegeneration

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Syntenin-1 Exosome Biogenesis Modulation Therapy for Neurodegeneration

10-Dimension Rubric Scoring

flowchart TD ideas_payload_syntenin_1_exoso["Syntenin-1 Exosome Biogenesis Modulation Therapy"] style ideas_payload_syntenin_1_exoso fill:#4fc3f7,stroke:#333,color:#000 ideas_payload_synten_0["10-Dimension Rubric Scoring"] ideas_payload_syntenin_1_exoso -->|"includes"| ideas_payload_synten_0 style ideas_payload_synten_0 fill:#81c784,stroke:#333,color:#000 ideas_payload_synten_1["Disease Coverage Matrix"] ideas_payload_syntenin_1_exoso -->|"includes"| ideas_payload_synten_1 style ideas_payload_synten_1 fill:#ef5350,stroke:#333,color:#000 ideas_payload_synten_2["Category"] ideas_payload_syntenin_1_exoso -->|"includes"| ideas_payload_synten_2 style ideas_payload_synten_2 fill:#ffd54f,stroke:#333,color:#000 ideas_payload_synten_3["Therapeutic Target"] ideas_payload_syntenin_1_exoso -->|"includes"| ideas_payload_synten_3 style ideas_payload_synten_3 fill:#ce93d8,stroke:#333,color:#000 ideas_payload_synten_4["Primary Target: Syntenin-1 SDCBP"] ideas_payload_syntenin_1_exoso -->|"includes"| ideas_payload_synten_4 style ideas_payload_synten_4 fill:#4fc3f7,stroke:#333,color:#000 ideas_payload_synten_5["Secondary Targets"] ideas_payload_syntenin_1_exoso -->|"includes"| ideas_payload_synten_5 style ideas_payload_synten_5 fill:#81c784,stroke:#333,color:#000

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Syntenin-1 Exosome Biogenesis Modulation Therapy for Neurodegeneration

10-Dimension Rubric Scoring

Mermaid diagram (expand to render)

| Dimension | Score | Rationale |
|-----------|-------|-----------|
| Novelty | 9/10 | First therapeutic targeting Syntenin-1/exosome biogenesis pathway; no existing therapies target this upstream exosome formation mechanism |
| Mechanistic Rationale | 8/10 | Strong mechanistic link: Syntenin-1 acts as master scaffold for ALIX-dependent exosome biogenesis; alpha-syn, tau, TDP-43 all shown to propagate via exosomes |
| Root-Cause Coverage | 7/10 | Addresses upstream mechanism of pathogenic protein secretion rather than downstream aggregation; reduces exosomal propagation burden |
| Delivery Feasibility | 7/10 | Small molecule inhibitors or peptide blockers could cross BBB; AAV-mediated shRNA possible but requires optimization |
| Safety Plausibility | 7/10 | Exosome biogenesis inhibition must be carefully titrated to avoid impairing normal neuronal communication; therapeutic window exists |
| Combinability | 8/10 | Synergizes with aggregation inhibitors, autophagy enhancers, and microglia modulators; addresses secretion component of proteostasis |
| Biomarker Availability | 6/10 | Exosomal protein cargo (p-tau, alpha-syn, TDP-43) in CSF/blood as pharmacodynamic markers; Syntenin-1 levels in extracellular vesicles |
| De-risking Path | 7/10 | In vitro proof in neuron cultures, ex vivo patient-derived iPSC neurons, then IND-enabling studies; clear readouts available |
| Multi-disease Potential | 9/10 | Core mechanism relevant to AD (tau exosomal spread), PD (alpha-syn exosomal spread), ALS (TDP-43 exosomal spread), FTD (TDP-43/tau) |
| Patient Impact | 8/10 | Addresses progressive spread of pathology; could slow disease progression in early-to-moderate stage patients |

Total Score: 76/100

Disease Coverage Matrix

| Disease | Coverage Score | Rationale |
|---------|----------------|-----------|
| Alzheimer's Disease | 9 | Tau propagation via exosomes well-documented; Syntenin-1 modulates this pathway |
| Parkinson's Disease | 9 | α-Synuclein secreted via exosomes; Syntenin-1 inhibition reduces burden |
| ALS | 8 | TDP-43 and SOD1 exported in exosomes; pathway relevance established |
| FTD | 8 | TDP-43 and tau propagation; shared exosomal mechanisms |
| Aging | 7 | Exosome biogenesis dysregulation with age; contributes to proteostatic decline |

Therapeutic Target

Primary Target: Syntenin-1 (SDCBP)

Syntenin-1 (also known as SDCBP) is a small PDZ domain-containing scaffold protein that plays a critical role in exosome biogenesis by recruiting ALIX to intraluminal vesicles (ILVs) in multivesicular bodies (MVBs).

Secondary Targets

ALIX (PD6A) — Essential cofactor for Syntenin-1-dependent exosome formation
ESCRT-III subunits (CHMP4B/C, CHMP2A) — Downstream effectors of exosome release
RAB27A/B — Regulators of MVB docking and exosome release (alternative pathway)

Key Mechanism

The Syntenin-ALIX Exosome Biogenesis Pathway

Syntenin-1 Recruitment: Syntenin-1 binds to phosphatidylinositol-4,5-bisphosphate (PIP2) on endosomal membranes via its N-terminal domain

ALIX Recruitment: Syntenin-1's PDZ domains recruit ALIX (also known as PD6A) through direct protein-protein interaction

ESCRT-III Recruitment: ALIX recruits ESCRT-III subunits (CHMP4B/C, CHMP2A) to facilitate membrane scission

MVB-Exosome Release: The MVB fuses with the plasma membrane, releasing exosomes into the extracellular space

Pathogenic Cargo Loading: Disease-associated proteins (α-syn, tau, TDP-43, SOD1) are selectively packaged into exosomes during this process

Therapeutic Intervention Points

Syntenin-1 small molecule inhibitors — Block PDZ domain interactions with ALIX
ALIX inhibitors — Prevent Syntenin-ALIX complex formation
Peptide blockers — Synthetic peptides mimicking Syntenin-1's ALIX-binding motif
RNAi/shRNA — Reduce Syntenin-1 expression via AAV-delivered constructs

Evidence for Therapeutic Relevance

[Roux et al., 2006](https://pubmed.ncbi.nlm.nih.gov/16543458/) — Original identification of Syntenin-1 as ALIX interactor via BioID
[Baietti et al., 2012](https://pubmed.ncbi.nlm.nih.gov/22903299/) — Demonstrated Syntenin-SPDP is required for exosome biogenesis in HeLa cells
[Larios et al., 2020](https://pubmed.ncbi.nlm.nih.gov/32439764/) — Confirmed ALIX- and ESCRT-III-dependent sorting of transmembrane proteins into exosomes
[Gauthier et al., 2017](https://pubmed.ncbi.nlm.nih.gov/28733926/) — Phosphorylated tau interacts with endosomal system and is secreted in exosomes
[Emmanouilidou et al., 2010](https://pubmed.ncbi.nlm.nih.gov/21177974/) — Cell-produced α-syn is secreted in exosomes in a calcium-dependent manner
[Schneider & Simons, 2016](https://pubmed.ncbi.nlm.nih.gov/27797869/) — Exosomes as vehicle for tau propagation between neurons

Rationale

Why This Target?

Upstream Mechanism: Unlike downstream aggregation inhibitors, this approach reduces the production of pathogenic exosomes at source

Genetic Validation: SDCBP (Syntenin-1) is widely expressed in neurons and glia; no known loss-of-function disease mutations suggest therapeutic inhibition is tolerable

Broad Disease Relevance: All major neurodegenerative proteinopathies involve exosomal propagation

Proof-of-Concept: Studies show reducing exosome release decreases pathological spreading in cell and animal models

Comparison to Existing Approaches

| Approach | Mechanism | Limitation |
|----------|-----------|------------|
| Aggregation inhibitors | Block protein aggregation | Doesn't address already-secreted seeds |
| Autophagy enhancers | Increase intracellular clearance | Doesn't reduce secretion |
| Antibody-based immunotherapies | Clear extracellular protein | Requires ongoing administration |
| Syntenin-1 modulation | Reduce exosome production | Novel, requires proof-of-concept |

Combination Therapy Potential

Synergistic Combinations

Syntenin-1 Modulation + Autophagy Induction

Syntenin-1 inhibition reduces exosomal secretion
Autophagy enhancers increase intracellular clearance
Combined effect: Reduced pathological burden from both secretion and accumulation

Syntenin-1 Modulation + Aggregation Inhibitors

Exosome reduction + intracellular aggregation prevention
Two-pronged attack on proteostasis

Syntenin-1 Modulation + Microglia State Editing

Reduces exosomal burden on microglia
TREM2-LXR modulation improves microglial clearance
Synergistic restoration of proteostasis

De-risking Path

Preclinical Development

In vitro proof-of-concept (Year 1)

Screen small molecule inhibitors of Syntenin-1 PDZ domains
Test in neuron/iPSC cultures from AD/PD patients
Measure exosomal tau/α-syn secretion via ELISA/Western blot

Ex vivo validation (Year 1-2)

Patient-derived iPSC neurons
Measure reduction in exosomal pathogenic cargo
Confirm viability and normal cellular function

IND-enabling studies (Year 2)

GMP synthesis of lead compound
PK/PD studies in relevant species
GLP toxicology (rodent + non-rodent)

Clinical Development

Phase I (Year 3)

Single ascending dose in healthy volunteers
Safety, PK, target engagement biomarkers

Phase II (Year 3-4)

Biomarker-enriched patient population
Primary endpoint: Reduction in CSF exosomal p-tau/α-syn
Secondary: Clinical efficacy signals

Implementation Roadmap

Immediate Actions (0-6 months)

Establish Syntenin-1 assay for small molecule screening

Develop cell-based reporter for exosome release

Screen compound libraries (FDA-approved drugs, natural products)

Identify lead candidates

Near-term Goals (6-18 months)

Optimize lead compounds for BBB penetration

Establish in vivo PK/PD correlation

Conduct proof-of-concept studies in APP/PS1 or α-syn transgenic mice

Measure exosomal tau/α-syn in brain and CSF

Long-term Goals (18-36 months)

IND submission

Initiate clinical trials

Establish biomarker platform for patient selection

Risk Assessment

| Risk | Likelihood | Mitigation |
|------|------------|------------|
| Insufficient BBB penetration | Medium | Use medicinal chemistry to optimize logP and polar surface area |
| Excessive exosome inhibition | Medium | Dose-finding with therapeutic window; titrate to partial inhibition |
| Off-target effects | Low | Selectivity screening; PDZ domain isoform selectivity |
| Lack of efficacy in humans | Unknown | Use patient-derived iPSCs for validation; biomarker enrichment |

References

[Roux et al., BioID identifies proximal proteins (2006)](https://pubmed.ncbi.nlm.nih.gov/16543458/)

[Baietti et al., Syntenin-ALIX exosome biogenesis (2012)](https://pubmed.ncbi.nlm.nih.gov/22903299/)

[Larios et al., ALIX-ESCRT-III sorting (2020)](https://pubmed.ncbi.nlm.nih.gov/32439764/)

[Gauthier et al., Tau in exosomes (2017)](https://pubmed.ncbi.nlm.nih.gov/28733926/)

[Emmanouilidou et al., α-Syn exosome secretion (2010)](https://pubmed.ncbi.nlm.nih.gov/21177974/)

[Schneider & Simons, Exosomes in tau propagation (2016)](https://pubmed.ncbi.nlm.nih.gov/27797869/)

[Exosome Biogenesis Mechanism](/mechanisms/exosome-biogenesis)
[Extracellular Vesicles in Neurodegeneration](/mechanisms/extracellular-vesicles)
[Alpha-Synuclein Exosomal Secretion](/mechanisms/alpha-synuclein-exosomal-secretion)
[Tau Propagation Pathways](/mechanisms/tau-propagation)
[ESCRT-III Neuroprotection Therapy](/ideas/payload-escrthost-III-neuroprotection-therapy)
[Extracellular Vesicle Neuroprotective Therapy](/ideas/extracellular-vesicle-neuroprotective-therapy)

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📊 Evidence Profile Foundational

Evidence Balance

+0%

Certainty

100%

Debates

0

Incoming

547

Outgoing

706

0 supporting 0 contradicting 0 neutral

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📗 Cite This Artifact

Syntenin-1 Exosome Biogenesis Modulation Therapy for Neurodegeneration

Syntenin-1 Exosome Biogenesis Modulation Therapy for Neurodegeneration

10-Dimension Rubric Scoring

Syntenin-1 Exosome Biogenesis Modulation Therapy for Neurodegeneration

10-Dimension Rubric Scoring

Disease Coverage Matrix

Category

Therapeutic Target

Primary Target: Syntenin-1 (SDCBP)

Secondary Targets

Key Mechanism

The Syntenin-ALIX Exosome Biogenesis Pathway

Therapeutic Intervention Points

Evidence for Therapeutic Relevance

Rationale

Why This Target?

Comparison to Existing Approaches

Combination Therapy Potential

Synergistic Combinations

De-risking Path

Preclinical Development

Clinical Development

Implementation Roadmap

Immediate Actions (0-6 months)

Near-term Goals (6-18 months)

Long-term Goals (18-36 months)

Risk Assessment

References

💬 Discussion

📗 Cite This Artifact

Syntenin-1 Exosome Biogenesis Modulation Therapy for Neurodegeneration

Syntenin-1 Exosome Biogenesis Modulation Therapy for Neurodegeneration

10-Dimension Rubric Scoring

Syntenin-1 Exosome Biogenesis Modulation Therapy for Neurodegeneration

10-Dimension Rubric Scoring

Disease Coverage Matrix

Category

Therapeutic Target

Primary Target: Syntenin-1 (SDCBP)

Secondary Targets

Key Mechanism

The Syntenin-ALIX Exosome Biogenesis Pathway

Therapeutic Intervention Points

Evidence for Therapeutic Relevance

Rationale

Why This Target?

Comparison to Existing Approaches

Combination Therapy Potential

Synergistic Combinations

De-risking Path

Preclinical Development

Clinical Development

Implementation Roadmap

Immediate Actions (0-6 months)

Near-term Goals (6-18 months)

Long-term Goals (18-36 months)

Risk Assessment

References

Related Pages

💬 Discussion