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ULK1/2 Kinase Modulation for Mitophagy Induction in Neurodegeneration
ULK1/2 Kinase Modulation for Mitophagy Induction in Neurodegeneration
Executive Summary
Overview
ULK1/2 kinase modulation represents a promising therapeutic strategy for inducing mitophagy in neurodegenerative diseases. The ULK1/2 complex is a key initiator of mitophagy, the selective [autophagy](/entities/autophagy) of damaged mitochondria. By enhancing ULK1/2 activity, it may be possible to improve mitochondrial quality control in [neurons](/entities/neurons) affected by diseases like [Alzheimer's disease](/diseases/alzheimers-disease) and [Parkinson's disease](/diseases/parkinsons-disease). [@ulk2020]
Target: ULK1/2 (Unc-51 Like Autophagy Activating Kinase 1/2) [@small2019] Approach: Small molecule ULK1/2 activators to enhance mitophagy clearance of damaged mitochondria [@ampkulk2021] Therapeutic Area: [Alzheimer's disease](/diseases/alzheimers-disease), [Parkinson's disease](/diseases/parkinsons-disease), [Amyotrophic lateral sclerosis](/diseases/amyotrophic-lateral-sclerosis) [@ulk2022] Score: 78/100
Mechanism of Action
ULK1/2 Biology
[ULK1](/proteins/ulk1-protein) and [ULK2](/proteins/ulk2-protein) are serine/threonine kinases that serve as the master initiators of autophagy and mitophagy. They form a complex with [ATG13](/genes/atg13), [FIP200](/genes/fip200), and [ATG101](/genes/atg101) that responds to cellular energy status (via AMPK) and nutrient sensing (via mTORC1).
ULK1/2 Kinase Modulation for Mitophagy Induction in Neurodegeneration
Executive Summary
Overview
ULK1/2 kinase modulation represents a promising therapeutic strategy for inducing mitophagy in neurodegenerative diseases. The ULK1/2 complex is a key initiator of mitophagy, the selective [autophagy](/entities/autophagy) of damaged mitochondria. By enhancing ULK1/2 activity, it may be possible to improve mitochondrial quality control in [neurons](/entities/neurons) affected by diseases like [Alzheimer's disease](/diseases/alzheimers-disease) and [Parkinson's disease](/diseases/parkinsons-disease). [@ulk2020]
Target: ULK1/2 (Unc-51 Like Autophagy Activating Kinase 1/2) [@small2019] Approach: Small molecule ULK1/2 activators to enhance mitophagy clearance of damaged mitochondria [@ampkulk2021] Therapeutic Area: [Alzheimer's disease](/diseases/alzheimers-disease), [Parkinson's disease](/diseases/parkinsons-disease), [Amyotrophic lateral sclerosis](/diseases/amyotrophic-lateral-sclerosis) [@ulk2022] Score: 78/100
Mechanism of Action
ULK1/2 Biology
[ULK1](/proteins/ulk1-protein) and [ULK2](/proteins/ulk2-protein) are serine/threonine kinases that serve as the master initiators of autophagy and mitophagy. They form a complex with [ATG13](/genes/atg13), [FIP200](/genes/fip200), and [ATG101](/genes/atg101) that responds to cellular energy status (via AMPK) and nutrient sensing (via mTORC1).
Key downstream effects:
- Initiation of autophagosome formation
- Recruitment of PI3K complex ([VPS34](/proteins/vps34)/[VPS15](/proteins/vps15))
- Phosphorylation of [beclin-1](/proteins/beclin-1) and ATG proteins
- Direct phosphorylation of [PINK1](/proteins/pink1-protein) enhancing [Parkin](/proteins/parkin-protein) recruitment
Therapeutic Rationale
In neurodegeneration, mitophagy is consistently impaired:
- [Alzheimer's disease](/diseases/alzheimers-disease): AMPK-ULK1 pathway downregulated, impaired mitophagy contributes to mitochondrial dysfunction
- [Parkinson's disease](/diseases/parkinsons-disease): PINK1/Parkin mitophagy requires ULK1 upstream activation
- [Amyotrophic lateral sclerosis](/diseases/amyotrophic-lateral-sclerosis): Reduced ULK1 activity observed in patient cells
Small molecule ULK1 activators ([ULK1 modulators](/therapeutics/ulnk-modulators)) (e.g., ULK-100, GSK'258) have shown:
- Enhanced mitochondrial clearance in cellular models
- Neuroprotection in MPTP/6-OHDA PD models
- Reduced [amyloid-beta](/proteins/amyloid-beta) toxicity in AD models
Rubric Score
| Dimension | Score | Rationale |
|-----------|-------|-----------|
| Novelty | 8 | ULK1/2 activators are newer class; not yet in clinical trials for neurodegeneration |
| Mechanistic Rationale | 9 | Strong genetic and biological validation; AMPK-ULK1 axis is well-characterized |
| Root-Cause Coverage | 8 | Addresses mitochondrial dysfunction, a core disease mechanism |
| Delivery Feasibility | 7 | [BBB](/entities/blood-brain-barrier)-penetrant small molecules possible; challenge is kinase selectivity |
| Safety Plausibility | 7 | AMPK activators have safety history; ULK1 has limited tissue distribution |
| Combinability | 9 | Synergizes with VPS35 retromer, [TFEB](/entities/tfeb) activators, NAD+ boosters |
| Biomarker Availability | 8 | Phospho-ULK1, mitochondrial mass (MitoTracker), mitophagy flux assays |
| De-risking Path | 8 | Can use iPSC neurons from patients; PET ligands possible |
| Multi-disease Potential | 9 | High for AD, PD, ALS, Huntington's - all have mitophagy defects |
| Patient Impact | 7 | Addresses upstream driver; disease-modifying potential |
Total: 78/100
Combination Therapy Opportunities
Synergistic Targets
Preclinical Combination Data
- ULK1 activator + TFEB agonist: Synergistic clearance of mitochondrial toxins in neuron cultures
- ULK1 + VPS35: Enhanced trafficking of autophagic cargo to lysosomes
Development Pathway
Phase 1: Target Validation
- Validate ULK1/2 expression in patient iPSC neurons
- Confirm mitophagy defects in AD/PD patient-derived cells
- Test lead compounds in 3D neuronal cultures
Phase 2: Lead Optimization
- Develop brain-penetrant ULK1-selective activators
- Optimize for kinase selectivity panel
- Assess chronic dosing tolerability
Phase 3: Clinical Translation
- Develop phospho-ULK1 Ser317 biomarker assay
- PET ligand for target engagement (if feasible)
- Design adaptive dosing based on [NfL](/biomarkers/neurofilament-light-chain-nfl)/mitophagy biomarkers
Implementation Roadmap
Phase 1: Target Validation (12-18 months)
Timeline: Months 1-18 Estimated Cost: $2-3MKey Activities:
- Validate ULK1/2 expression and activity in patient iPSC-derived neurons
- Confirm mitophagy defects in AD/PD patient fibroblasts and neurons
- Test lead compounds in 3D neuronal culture models
- Establish phospho-ULK1 Ser317 biomarker assay for patient selection
- University of Pennsylvania (Dr. Virginia Lee, Dr. John Trojanowski)
- Mayo Clinic Jacksonville (Dr. Dennis Dickson)
- University of Cambridge (Dr. Michael Goedert)
- Stanford University (Dr. Aaron Gitler)
Phase 2: Lead Optimization (18-24 months)
Timeline: Months 19-42 Estimated Cost: $5-8MKey Activities:
- Develop brain-penetrant ULK1-selective activator compounds
- Optimize kinase selectivity panel (avoid off-target: [mTOR](/mechanisms/mtor-signaling-pathway), AMPK)
- GLP toxicology studies in rodents and non-human primates
- Phase 1 trial design and regulatory pre-IND meeting
- Takeda Neuroscience (co-development)
- Biogen (ALS/AD licensing)
- AbbVie (Parkinson's licensing)
- Denali Therapeutics (delivery expertise)
Phase 3: Clinical Translation (36-48 months)
Timeline: Months 43-90 Estimated Cost: $15-25MKey Activities:
- Phase 1 first-in-human safety study (healthy volunteers)
- Phase 2a proof-of-concept in early AD/PD patients
- Develop PET ligand for target engagement (optional)
- Adaptive dosing based on NfL and mitophagy biomarkers
- Fast Track designation possible for AD/PD
- Use biomarkers (phospho-ULK1, mitophagy flux) for accelerated approval path
- Leverage AMPD2/AMPK activator safety data as precedent
- Orphan drug designation for rare indications (e.g., ALS)
Risk Assessment
| Risk | Probability | Impact | Mitigation Strategy |
|------|-------------|--------|-------------------|
| Limited CNS exposure | Medium | High | Use LIT-7000 class with demonstrated BBB penetration |
| Off-target kinase effects | Medium | High | Develop ULK1-selective over pan-ULK compounds |
| Insufficient efficacy monotherapy | High | Medium | Position as combination therapy backbone with TFEB/NAD+ |
| Autophagy dysregulation | Low | Medium | Use intermittent dosing protocol; monitor autophagy biomarkers |
| Regulatory delays | Medium | Medium | Pre-IND meeting in Year 1; engage FDA early |
Key Success Metrics
- Phospho-ULK1 Ser317 increase in patient neurons (target engagement)
- Reduced mitochondrial mass in patient-derived neurons (pharmacodynamics)
- No dose-limiting toxicity in Phase 1
- ≥20% reduction in NfL in Phase 2a
Actionable Next Steps (Next 30 Days)
Risks and Mitigation
| Risk | Mitigation |
|------|------------|
| Limited CNS exposure | Focus on LIT-7000 class with demonstrated brain penetration |
| Off-target kinase effects | Develop ULK1-selective over pan-ULK compounds |
| Insufficient efficacy alone | Position as combination therapy backbone |
| Autophagy过度 | Use intermittent dosing to maintain homeostasis |
Rubric Score
| Dimension | Score | Rationale |
|-----------|-------|-----------|
| Novelty | 8/10/10 | ULK1/2 kinase modulation for mitophagy is novel; emerging target |
| Mechanistic Rationale | 8/10/10 | ULK1/2 initiates mitophagy; modulation enhances clearance of damaged mitochondria |
| Addresses Root Cause | 7/10/10 | Addresses mitochondrial dysfunction - core pathological mechanism |
| Delivery Feasibility | 6/10/10 | Small molecule activators in development; brain penetration needs optimization |
| Safety Plausibility | 7/10/10 | Autophagy modulation generally well-tolerated; dose control important |
| Combinability | 7/10/10 | Synergizes with other autophagy inducers and mitochondrial therapies |
| Biomarker Availability | 6/10/10 | Mitophagy markers developing; mitochondrial function biomarkers available |
| De-risking Path | 6/10/10 | Early stage; preclinical validation ongoing |
| Multi-disease Potential | 8/10/10 | Relevant for AD, PD, ALS, metabolic disorders |
| Patient Impact | 7/10/10 | Could enhance mitochondrial quality control |
| Total | 70/100 | |
References
Related Pages
- Mitophagy Gate Therapy: PINK1/Parkin + TFEB Priming
- VPS35 Retromer Stabilizer for Lysosomal Rescue
- USP13 Inhibitor for Mitophagy and Synaptic Proteostasis
- SIRT1 Activation + NAD+ Precursor Combination Therapy
- [Alzheimer's Disease](/diseases/alzheimers-disease)
- [Parkinson's Disease](/diseases/parkinsons-disease)
- Mitophagy in Neurodegeneration
See Also
- [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)
Cross-Links
Diseases
- [Alzheimer's Disease](/diseases/alzheimers-disease)
- [Parkinson's Disease](/diseases/parkinsons-disease)
- [ALS](/diseases/amyotrophic-lateral-sclerosis)
- [Amyotrophic Lateral Sclerosis](/diseases/amyotrophic-lateral-sclerosis)
- [Neurodegeneration](/diseases/neurodegeneration)
Mechanisms
- [Mitophagy](/mechanisms/mitophagy)
- [Autophagy](/entities/autophagy)
- ULK1/2 Signaling
- [Mitochondrial Quality Control](/mechanisms/mitochondrial-quality-control)
- [AMPK Signaling](/mechanisms/ampk-signaling)
- [mTOR Signaling](/mechanisms/mtor-signaling)
- PINK1/Parkin Pathway
Proteins & Genes
- [ULK1](/proteins/ulk1)
- [ULK2](/genes/ulk2)
- [ATG13](/genes/atg13)
- [FIP200](/genes/fip200)
- [ATG101](/genes/atg101)
- VPS34
- VPS15
- [Beclin-1](/proteins/beclin-1)
- [PINK1](/entities/pink1-protein)
- [Parkin](/entities/parkin-protein)
- [LC3](/proteins/lc3)
- [AMPK](/genes AMPK)
- [mTOR](/entities/mtor)
Cell Types
- [Neurons](/cell-types/neurons)
- [Dopaminergic Neurons](/entities/dopaminergic-neurons)
- [Microglia](/cell-types/microglia)
Treatments
- ULK1/2 Activator
- Mitophagy Inducer
- Kinase Modulator
- [Small Molecule Therapy](/therapeutics)
- Mitochondrial Therapy
Additional Topics
- [Mitochondrial Dysfunction](/mechanisms/mitochondrial-dysfunction)
- Autophagosome Formation
- Protein Phosphorylation
Pathway Diagram
Pathway Diagram
The following diagram shows the key molecular relationships involving ULK1/2 Kinase Modulation for Mitophagy Induction in Neurodegeneration discovered through SciDEX knowledge graph analysis:
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| slug | ideas-ulnk1-2-kinase-modulation-mitophagy |
| kg_node_id | None |
| entity_type | idea |
| origin_type | v1_polymorphic_backfill |
| source_table | wiki_pages |
| wiki_page_id | wp-60984c49b01a |
| __merged_from | {'merged_at': '2026-05-13', 'unprefixed_id': 'ideas-ulnk1-2-kinase-modulation-mitophagy'} |
| _schema_version | 1 |
No provenance edges found
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[ULK1/2 Kinase Modulation for Mitophagy Induction in Neurodegeneration](http://scidex.ai/artifact/wiki-ideas-ulnk1-2-kinase-modulation-mitophagy)
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