AAV-LRRK2 IND-Enabling Study Design

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experiment1843 wordssynced 2026-04-02

Experiment Category: Gene Therapy / IND-Enabling Preclinical Studies Created: 2026-03-21 Based on: AAV Serotype Comparison for [LRRK2](/entities/lrrk2) (/experiments/aaav-serotype-comparison-lrrk2)

Executive Summary

This document outlines comprehensive IND-enabling preclinical studies for AAV-LRRK2 gene therapy targeting Parkinson's disease. Building on our serotype comparison results demonstrating AAV-PHP.B as the optimal vector, we propose a complete package including GLP toxicology, biodistribution, dose escalation, and long-term NHP safety studies to support an IND submission to the FDA.

Background and Rationale

LRRK2 (Leucine-Rich Repeat Kinase 2) mutations are the most common cause of autosomal-dominant Parkinson's disease, accounting for 5-10% of familial PD cases. Our prior serotype comparison study identified AAV-PHP.B as demonstrating superior transduction efficiency and reduced immunogenicity compared to traditional serotypes (AAV2, AAV5, AAV9) in both mouse and NHP brain tissue.

The IND-enabling studies outlined below are designed to generate the safety, toxicity, and efficacy data required by FDA 21 CFR 312.23 for a gene therapy IND application.

Study 1: GLP Single-Dose Toxicology Study

Study Objectives

Evaluate the safety and tolerability of a single intracerebral dose of AAV-PHP.B-shLRRK2 in rats and non-human primates
Identify target organs, dose-limiting toxicities, and maximum tolerated dose (MTD)
Generate GLP-compliant data for IND submission

Study Design

...

Executive Summary

Background and Rationale

The IND-enabling studies outlined below are designed to generate the safety, toxicity, and efficacy data required by FDA 21 CFR 312.23 for a gene therapy IND application.

Study 1: GLP Single-Dose Toxicology Study

Study Objectives

Evaluate the safety and tolerability of a single intracerebral dose of AAV-PHP.B-shLRRK2 in rats and non-human primates
Identify target organs, dose-limiting toxicities, and maximum tolerated dose (MTD)
Generate GLP-compliant data for IND submission

Study Design

| Parameter | Rats | Non-Human Primates |
|-----------|------|-------------------|
| Species | Sprague-Dawley | Cynomolgus macaques |
| Age | 8-10 weeks | 3-5 years |
| Groups | 4 (3 dose + 1 control) | 4 (3 dose + 1 control) |
| Males/Females | 10/sex/group | 3/sex/group |
| Doses | Low: 1×10^13 GC, Mid: 3×10^13 GC, High: 1×10^14 GC | Low: 1×10^13 GC, Mid: 3×10^13 GC, High: 1×10^14 GC |
| Route | Intracerebral (stereotactic) | Intracerebral (stereotactic) |
| Observation | 28 days | 90 days |

Primary Endpoints

Clinical observations (neurological, behavioral, physical)
Body weight and food consumption
Clinical pathology (hematology, clinical chemistry, coagulation)
Gross necropsy and organ weights
Histopathology (including brain, liver, kidney, spleen, heart, lung)
Immunogenicity (anti-AAV antibodies, T-cell responses)

Secondary Endpoints

Biodistribution (qPCR for vector genome copy number)
LRRK2 mRNA expression in target tissues
Biomarker analysis ([NfL](/biomarkers/neurofilament-light-chain-nfl), [tau](/proteins/tau), [α-synuclein](/proteins/alpha-synuclein) in CSF)
Cytokine/chemokine panels

Budget Estimate

| Item | Cost |
|------|------|
| GLP study contract (CRO) | $450,000 |
| Vector production (GLP grade) | $120,000 |
| Histopathology | $85,000 |
| Bioanalysis | $65,000 |
| Report writing | $35,000 |
| Total | $755,000 |

Study 2: Biodistribution Study

Study Objectives

Determine vector genome distribution following intracerebral administration
Identify off-target tissues and persistence
Characterize shedding characteristics

Study Design

| Parameter | Mice | NHPs |
|-----------|------|------|
| Species | C57BL/6 | Cynomolgus macaques |
| Groups | 5 timepoints | 3 timepoints |
| Timepoints | 1, 7, 28, 90, 180 days | 7, 90, 180 days |
| Tissues collected | 25 tissues | 30 tissues |
| Samples per timepoint | 10 animals | 3 animals |

Tissues to Analyze

Brain (injected region, contralateral, [cortex](/brain-regions/cortex), cerebellum)
Spinal cord
Liver
Spleen
Kidney
Heart
Lung
Testis/Ovary
Drainage lymph nodes
Blood (plasma, PBMCs)

Analytical Methods

Droplet digital PCR (ddPCR) for vector genome quantification
RNAseq for transcriptional changes
ELISA for protein expression

Budget Estimate

| Item | Cost |
|------|------|
| Vector production | $50,000 |
| Tissue processing | $35,000 |
| ddPCR analysis | $45,000 |
| RNAseq | $30,000 |
| Report | $15,000 |
| Total | $175,000 |

Study 3: Dose-Range Finding Study

Study Objectives

Establish dose-response relationship for efficacy
Identify no-observed-adverse-effect level (NOAEL)
Support dose selection for pivotal studies

Study Design

| Parameter | Rats |
|-----------|------|
| Groups | 5 (4 dose + 1 vehicle) |
| Dose range | 1×10^11 to 1×10^14 GC |
| Route | Intracerebral |
| Duration | 90 days |
| Animals | 15/sex/group |

Efficacy Readouts

LRRK2 mRNA knockdown (qPCR)
LRRK2 protein expression (Western blot, IHC)
Tyrosine hydroxylase (TH) neuron survival
Behavioral testing (cylinder, rotarod, gait analysis)
Neuroinflammation markers (Iba1, GFAP)

Budget Estimate

| Item | Cost |
|------|------|
| Vector production | $80,000 |
| In-life phase | $95,000 |
| Tissue analysis | $55,000 |
| Behavioral testing | $25,000 |
| Report | $20,000 |
| Total | $275,000 |

Study 4: Long-Term NHP Safety Study

Study Objectives

Evaluate safety of long-term LRRK2 knockdown
Assess durability of therapeutic effect
Characterize late-onset toxicity (12 months)

Study Design

| Parameter | Specification |
|-----------|---------------|
| Species | Cynomolgus macaques |
| Groups | 4 (3 dose + 1 control) |
| Doses | Low: 1×10^13 GC, Mid: 3×10^13 GC, High: 1×10^13 GC |
| Animals | 6/sex/group (48 total) |
| Duration | 12 months |
| Route | Bilateral intraparenchymal (SNc + striatum) |

Enhanced Monitoring

Monthly neurological examinations
Quarterly CSF collection (cell count, protein, NfL, tau, α-syn)
PET imaging (DAT, TH) at baseline, 6, 12 months
Comprehensive behavioral assessment

Histopathology Battery

Full neural axis examination
Peripheral organ toxicity
Reproductive organ assessment
Electron microscopy of target [neurons](/entities/neurons)

Budget Estimate

| Item | Cost |
|------|------|
| NHP procurement & holding | $720,000 |
| Vector production | $180,000 |
| In-life monitoring | $250,000 |
| Imaging (PET) | $120,000 |
| CSF analysis | $85,000 |
| Histopathology | $150,000 |
| Bioanalysis | $75,000 |
| Report writing | $60,000 |
| Total | $1,640,000 |

Manufacturing Scale-Up Plan

Current State (Research Grade)

Production scale: 1-5 × 10^14 GC per batch
System: Triple transfection in HEK293 cells
Purification: CsCl gradient or affinity chromatography

Target State (GMP Grade)

Production scale: 1-5 × 10^16 GC per batch
Scale-up pathway:

| Phase | Scale | Timeline | Purpose |
|-------|-------|----------|---------|
| Pilot | 10^15 GC | Months 1-3 | Process development |
| Demo | 5×10^15 GC | Months 4-6 | Validation batches |
| GMP Batch 1 | 1×10^16 GC | Months 7-9 | GLP toxicology |
| GMP Batch 2 | 1×10^16 GC | Months 10-12 | Pivotal studies |
| GMP Batch 3 | 1×10^16 GC | Months 13-15 | IND filing |

Manufacturing Partners (Pre-qualified)

| Company | Location | Capability |
|---------|----------|------------|
| Vigene Biosciences | USA (MD) | AAV GMP, 200L+ |
| Catalent | USA (NJ) | AAV GMP, 1000L |
| Oxford BioMedica | UK | Lentivirus/AAV GMP |
| Thermo Fisher | USA | GMP manufacturing |
| Charles River Labs | USA | GLP/GMP toxicology |

CMC Requirements for IND

| Requirement | Specification |
|-------------|---------------|
| Identity | Sequencing, restriction analysis |
| Purity | >95% empty capsids, <3% host cell DNA |
| Potency | Transduction units (TU) per mL |
| Stability | 24 months at -80°C |
| Sterility | No growth in sterility tests |
| Endotoxin | <0.5 EU/mL |

Manufacturing Cost Estimate

| Item | Cost |
|------|------|
| Process development | $200,000 |
| GMP vector production (3 batches) | $600,000 |
| Analytical testing | $150,000 |
| Fill/finish | $75,000 |
| Stability studies | $100,000 |
| Quality release | $50,000 |
| Total | $1,175,000 |

Regulatory Strategy

Regulatory Pathway

Product Type: Gene therapy (AAV vector)
Route: Intracerebral (intraparenchymal)
Classification: Biological, Section 351(a) (Live recombinant virus)
FDA Division: Center for Biologics Evaluation and Research (CBER)

Pre-IND Package

| Document | Status | Timeline |
|----------|--------|----------|
| Product description | To be prepared | Month 1-2 |
| Manufacturing summary | To be prepared | Month 1-3 |
| Preclinical data package | To be prepared | Month 3-6 |
| IND application | To be filed | Month 9 |

Pre-IND Meeting Request

Timing: Prior to IND submission
Topics: Study design, CMC requirements, regulatory expectations
FDA Office: Office of Cellular, Tissue, and Gene Therapies (OCTGT)

Key Regulatory Considerations

Efficacy Endpoints: Discuss with FDA on appropriate biomarkers vs. clinical endpoints

Animal Model Requirements: Demonstrate relevance to human disease

Dose Selection: Provide scientific rationale based on NHP data

Manufacturing Changes: Minimize between toxicology and clinical batches

Risk Mitigation: Immune response management strategy

Regulatory Timeline

| Milestone | Target Date |
|-----------|-------------|
| Pre-IND meeting | Month 6 |
| IND submission | Month 9 |
| IND clearance | Month 12 |
| First patient dosing | Month 15 |

Estimated Regulatory Costs

| Item | Cost |
|------|------|
| Regulatory consulting | $75,000 |
| Pre-IND meeting preparation | $25,000 |
| IND application assembly | $35,000 |
| FDA user fees | $2,478 (IND) |
| Post-IND support | $50,000 |
| Total | $187,478 |

Integrated Timeline

gantt
title AAV-LRRK2 IND-Enabling Studies Timeline
dateFormat YYYY-MM
section Manufacturing
Process Development :2026-04, 3
GMP Production Batch 1 :2026-07, 3
GMP Production Batch 2 :2026-10, 3
GMP Production Batch 3 :2027-01, 3
section GLP Toxicology
Single-Dose Toxicology :2026-07, 6
Long-Term NHP Study :2026-10, 12
section Other Studies
Biodistribution :2026-07, 6
Dose-Range Finding :2026-07, 4
section Regulatory
Pre-IND Meeting :2026-09, 1
IND Submission :2026-12, 1

Total Budget Summary

| Category | Cost |
|----------|------|
| GLP Toxicology | $755,000 |
| Biodistribution | $175,000 |
| Dose-Range Finding | $275,000 |
| Long-Term NHP Safety | $1,640,000 |
| Manufacturing | $1,175,000 |
| Regulatory | $187,000 |
| TOTAL | $4,207,000 |

Risk Assessment and Mitigation

| Risk | Probability | Impact | Mitigation |
|------|-------------|--------|------------|
| NHP study delays | Medium | High | Contingency timeline, alternative CRO |
| Manufacturing failure | Low | High | Dual sourcing, process robustness |
| Regulatory hold | Low | High | Pre-IND communication, robust data |
| Immune response | Medium | Medium | Immunomodulation protocol |
| Efficacy signal weak | Medium | High | Dose optimization, alternative constructs |

Cross-Links to NeuroWiki Pages

[LRRK2](/genes/lrrk2) - Target gene
[LRRK2 Protein](/proteins/lrrk2-protein) - Protein product
[Parkinson's Disease](/diseases/parkinsons-disease) - Target disease
[AAV Vectors for Neurodegenerative Gene Therapy](/therapeutics/aav-vectors-neurodegenerative-gene-therapy) - Vector platform
[Gene Therapy for Parkinson's](/therapeutics/gene-therapy-parkinsons) - Related treatment
[G2019S LRRK2 Mutation](/diseases/lrrk2-g2019s-parkinsonism) - Common mutation
[AAV Serotype Comparison Experiment](/experiments/aaav-serotype-comparison-lrrk2) - Prior work

Conclusion

This comprehensive IND-enabling study package provides a clear path from our promising preclinical data to an FDA IND submission for AAV-LRRK2 gene therapy in Parkinson's disease. The total investment of approximately $4.2M over 15-18 months positions the program for clinical development with a well-characterized, safe, and effective gene therapy candidate.

External Links

[PubMed](https://pubmed.ncbi.nlm.nih.gov/)
[ClinicalTrials.gov](https://clinicaltrials.gov/)

References

Unknown, FDA Guidance: Gene Therapy Clinical Trials - Monitoring Participants (n.d.)

Unknown, FDA Guidance: Human Gene Therapy Products Incorporating Genome Editing (n.d.)

Unknown, ICH M3(R2) Guidance: Nonclinical Safety Studies for the Conduct of Human Clinical Trials (n.d.)

[Unknown, AAV Gene Therapy: Regulatory Considerations (Nature Reviews Drug Discovery) (n.d.)](https://doi.org/10.1038/s41573-021-00152-1)

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AAV-LRRK2 IND-Enabling Study Design

Executive Summary

Background and Rationale

Study 1: GLP Single-Dose Toxicology Study

Study Objectives

Study Design

Executive Summary

Background and Rationale

Study 1: GLP Single-Dose Toxicology Study

Study Objectives

Study Design

Primary Endpoints

Secondary Endpoints

Budget Estimate

Study 2: Biodistribution Study

Study Objectives

Study Design

Tissues to Analyze

Analytical Methods

Budget Estimate

Study 3: Dose-Range Finding Study

Study Objectives

Study Design

Efficacy Readouts

Budget Estimate

Study 4: Long-Term NHP Safety Study

Study Objectives

Study Design

Enhanced Monitoring

Histopathology Battery

Budget Estimate

Manufacturing Scale-Up Plan

Current State (Research Grade)

Target State (GMP Grade)

Manufacturing Partners (Pre-qualified)

CMC Requirements for IND

Manufacturing Cost Estimate

Regulatory Strategy

Regulatory Pathway

Pre-IND Package

Pre-IND Meeting Request

Key Regulatory Considerations

Regulatory Timeline

Estimated Regulatory Costs

Integrated Timeline

Total Budget Summary

Risk Assessment and Mitigation

Cross-Links to NeuroWiki Pages

Conclusion

See Also

External Links

References