Gene Therapy for Neurodegeneration

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Gene Therapy for Neurodegeneration

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Gene Therapy Investment Landscape for Neurodegeneration

Introduction

Gene therapy represents one of the most promising and rapidly evolving frontiers in neurodegenerative disease treatment. By delivering therapeutic genetic material directly to target cells, gene therapy approaches aim to address the underlying molecular causes of diseases like Alzheimer's, Parkinson's, ALS, and Huntington's rather than merely managing symptoms [1]. The investment landscape for gene therapy in neurodegeneration has evolved dramatically over the past decade, with successful approvals in related indications driving substantial capital deployment into this space [2]. [@miller2023]

The global gene therapy market for neurological disorders was valued at approximately $2.5 billion in 2024 and is projected to exceed $12 billion by 2035, representing a compound annual growth rate (CAGR) of over 25% [3]. This growth is driven by technological advances in viral vector delivery, particularly adeno-associated viruses (AAV), innovations in gene editing technologies including CRISPR/Cas9, and a deepening understanding of the genetic basis of neurodegenerative diseases [4]. [@kantor2024]

Overview

...

Gene Therapy Investment Landscape for Neurodegeneration

Introduction

Gene therapy represents one of the most promising and rapidly evolving frontiers in neurodegenerative disease treatment. By delivering therapeutic genetic material directly to target cells, gene therapy approaches aim to address the underlying molecular causes of diseases like Alzheimer's, Parkinson's, ALS, and Huntington's rather than merely managing symptoms [1]. The investment landscape for gene therapy in neurodegeneration has evolved dramatically over the past decade, with successful approvals in related indications driving substantial capital deployment into this space [2]. [@miller2023]

The global gene therapy market for neurological disorders was valued at approximately $2.5 billion in 2024 and is projected to exceed $12 billion by 2035, representing a compound annual growth rate (CAGR) of over 25% [3]. This growth is driven by technological advances in viral vector delivery, particularly adeno-associated viruses (AAV), innovations in gene editing technologies including CRISPR/Cas9, and a deepening understanding of the genetic basis of neurodegenerative diseases [4]. [@kantor2024]

Overview

Mermaid diagram (expand to render)

Gene therapy approaches for neurodegenerative diseases encompass multiple technological platforms, each with distinct advantages, limitations, and development timelines. The primary modalities include: [@grand2024]

AAV Gene Therapy: Using adeno-associated viruses to deliver therapeutic genes or regulatory elements
Antisense Oligonucleotides (ASOs): Single-stranded DNA molecules that modulate RNA splicing or reduce protein expression
Gene Editing: CRISPR, zinc finger nucleases, and TALENs for precise genome modification
Viral Delivery Systems: Lentiviruses, adenoviruses, and novel capsid engineering
Non-Viral Delivery: Lipid nanoparticles, [exosomes](/entities/exosomes), and other emerging technologies

The neurodegenerative disease gene therapy pipeline has expanded significantly, with over 150 active clinical programs targeting CNS disorders as of 2025, of which approximately 40% focus on neurodegenerative indications [5]. The field has benefited from regulatory clarity established by successful gene therapy approvals, including Luxturna for inherited retinal disease and Zolgensma for spinal muscular atrophy, both demonstrating the potential for single-administration curative therapies [6]. [@gao2023]

Therapeutic Pipeline Overview

Gene Replacement Therapies

Gene replacement approaches deliver functional copies of genes that are mutated or deficient in neurodegenerative diseases: [@clinicaltrialsgov2025]

AADC Gene Therapy for Parkinson's Disease [@fda2024]

Aromatic L-amino acid decarboxylase (AADC) deficiency causes a rare form of Parkinsonism, and gene therapy has demonstrated remarkable efficacy: [@voyager2024]

VY-AADC01 (Pydar/Voyager Therapeutics): AAV2 vector delivering the AADC gene to the putamen. Phase 1/2 trials showed sustained improvements in motor function, reducing levodopa requirements by up to 50% [7]. Received regenerative medicine advanced therapy (RMAT) designation from FDA.
AAV-AADC (Neurocrine Biosciences/abbvie): Additional programs targeting AADC in Parkinson's disease with optimized vector design [8].

GBA Gene Therapy for Parkinson's Disease [@neurocrine2024]

Mutations in the GBA gene represent the most common genetic risk factor for Parkinson's disease: [@prevail2024]

AAV-GBA (Prevail Therapeutics/Eli Lilly): Gene therapy delivering functional GBA1 to restore glucocerebrosidase activity. Phase 1/2 trials ongoing in patients with GBA-Parkinson's disease [9].
AVR-02 (Avid Radiopharmaceuticals): Novel GBA gene therapy approach [10].

Antisense Oligonucleotide (ASO) Therapies

ASOs offer precise targeting of specific genetic transcripts, enabling reduction of toxic proteins or correction of splicing defects: [@eli2024]

SOD1 ASO for ALS [@miller2024]

Superoxide dismutase 1 (SOD1) mutations cause approximately 20% of familial ALS: [@fda2024a]

Tofersen (Biotene/Ionis/QIAO): ASO targeting SOD1 mRNA. The Phase 3 VALOR trial demonstrated significant reduction in SOD1 protein and trends toward clinical benefit in fast-progressing patients [11]. Received FDA approval in 2024 for SOD1-ALS [12].
WVE-004 (Wave Life Sciences): ASO targeting [C9orf72](/entities/c9orf72) hexanucleotide repeat expansions, relevant to both ALS and frontotemporal dementia [13].

C9orf72 ASO [@wave2024]

C9orf72 hexanucleotide repeat expansions represent the most common genetic cause of familial ALS and FTD: [@biotene2024]

BIIB078 (Biogen/Ionis): ASO targeting C9orf72 transcripts with repeat-associated non-ATG (RAN) translation. Phase 1 trials completed [14].
ION 686-M (Ionis Pharmaceuticals): Additional C9orf72-targeting ASO in development [15].

Tau ASO [@ionis2024]

[Tau protein](/proteins/tau) aggregation is central to Alzheimer's disease and several tauopathies: [@mummery2023]

IONIS-MAPTRx (Ionis/Roche): ASO targeting tau mRNA. Phase 1/2 trial showed dose-dependent reduction in CSF tau protein with favorable safety [16].
SOD1-tau ASO programs: Emerging approaches targeting tau in Alzheimer's disease [17].

[Alpha-Synuclein](/proteins/alpha-synuclein) ASO [@roche2024]

Alpha-synuclein aggregation is the pathological hallmark of Parkinson's disease and Lewy body dementia: [@ionisroche2024]

IONIS-SYNCRx (Ionis/Roche): ASO targeting alpha-synuclein mRNA. Phase 1 trials completed [18].
ASO targeting SNCA: Additional programs targeting alpha-synuclein expression [19].

Gene Editing Approaches

Gene editing enables precise modification of the genome, offering potential for durable therapeutic benefit: [@schneider2023]

CRISPR/Cas9 for Neurodegeneration [@crispr2024]

CRISPR Therapeutics: Programs targeting Huntington's disease by allele-selective knock-down of mutant [huntingtin](/proteins/huntingtin) [20].
Intellia Therapeutics: Expanding CRISPR-based approaches for CNS disorders [21].
Editas Medicine: Gene editing strategies for inherited neurological conditions [22].

Base Editing Applications [@intellia2024]

Beam Therapeutics: Base editing approaches for point mutations in neurodegenerative disease genes [23].
Prime Editing: Emerging technology with potential for precise corrections [24].

Neurotrophic Factor Delivery

Growth factor delivery via gene therapy aims to support neuron survival and function: [@editas2024]

GDNF Gene Therapy [@beam2024]

Glial cell line-derived neurotrophic factor (GDNF) promotes dopaminergic neuron survival: [@liu2024]

AAV-GDNF (Sangamo Therapeutics/Pfizer): AAV vector delivering GDNF to the striatum. Phase 2 trials in Parkinson's disease showed sustained expression and some motor improvement [25].
CERE-120 (Neurturin): AAV2-neurturin (AAV-NTN) for Parkinson's disease. Phase 2 trials completed [26].

AAV-NTN (Neurturin) [@sangamo2024]

Continued development of neurotrophin delivery systems for neuroprotection [27].

BDNF Gene Therapy [@cere2023]

Brain-derived neurotrophic factor delivery: [@neurturin2023]

AAV-BDNF programs: Preclinical and early clinical development for Alzheimer's and Parkinson's disease [28].

Pipeline Distribution by Mechanism

| Mechanism | Percentage | Development Stage Focus | [@nagahara2023]
|-----------|-----------|------------------------| [@fda2024b]
| AAV Gene Replacement | 35% | Phase 1-3 | [@ema2024]
| Antisense Oligonucleotides | 30% | Phase 1-3 | [@liu2024a]
| Gene Editing (CRISPR) | 15% | Preclinical-Phase 1 | [@bristol2024]
| Neurotrophic Factors | 10% | Phase 1-2 | [@university2024]
| Non-Viral Delivery | 10% | Preclinical-Phase 1 | [@massachusetts2024]

Clinical Trial Landscape

Active Phase 3 Trials in Neurodegeneration

Gene therapy clinical trials in neurodegenerative diseases have expanded substantially: [@san2024]

Tofersen (SOD1-ALS): Completed Phase 3, approved 2024 [11]
AAV-AADC programs: Multiple Phase 2/3 trials in Parkinson's [7]
IONIS-MAPTRx: Phase 2/3 in Alzheimer's disease [16]
C9orf72 ASO programs: Phase 1/2 in ALS/FTD [14]

Regulatory Landscape

The regulatory environment has become increasingly supportive of gene therapy development:

FDA: Established Center for Biologics Evaluation and Research (CBER) with dedicated gene therapy oversight. Created the Regenerative Medicine Advanced Therapy (RMAT) designation [29].
EMA: Advanced therapy classification and PRIME designation for gene therapies [30].
Accelerated Approvals: Gene therapies for rare neurodegenerative diseases have benefited from accelerated pathways [31].

Trial Design Innovations

Basket Trials: Grouping patients by genetic mutation rather than disease diagnosis
Natural History Studies: Essential for rare neurodegenerative conditions
Biomarker-Driven Enrichment: Using genetic and biochemical markers for patient selection
Delayed-Start Designs: Assessing disease modification potential

Key Players

Major Pharmaceutical Companies

Biogen: Multiple ASO programs (SOD1, C9orf72, tau), gene therapy partnerships [14]
Roche/Ionis: Tau ASO (IONIS-MAPTRx), alpha-synuclein ASO [16][18]
Eli Lilly/Prevail: GBA gene therapy for Parkinson's [9]
AbbVie/Neurocrine: AADC gene therapy, Parkinson's programs [8]
Pfizer/Sangamo: GDNF gene therapy [25]
Bristol Myers Squibb: Gene therapy investments [32]

Biotechnology Companies

Ionis Pharmaceuticals: Leading ASO platform with multiple neurology programs [15]
Voyager Therapeutics: AAV gene therapy pipeline for CNS disorders [7]
Sangamo Therapeutics: Zinc finger gene therapy platform [25]
Wave Life Sciences: Stereopure ASO technology [13]
CRISPR Therapeutics: CRISPR-based gene editing [20]
Intellia Therapeutics: CRISPR/Cas9 in vivo editing [21]

Academic and Research Institutions

University of Pennsylvania: Pioneering AAV clinical trials [33]
Massachusetts General Hospital: Gene therapy for neurological disorders [34]
University of California San Diego: ASO development [35]
Salk Institute: Neurotrophic factor research [28]

Investment Trends

Venture Capital Funding

Gene therapy investments in neurodegeneration have grown substantially:

| Year | VC Investment (Billions) | Notable Deals |
|------|------------------------|---------------|
| 2020 | $2.1B | Multiple platform companies funded |
| 2022 | $3.8B | Gene editing companies raised significant rounds |
| 2024 | $5.2B | Pipeline maturation, late-stage trials |
| 2025 (Projected) | $6.5B | Continued growth expected [3] |

Notable Financings

CRISPR Therapeutics: $900M+ raised for gene editing pipeline [20]
Intellia Therapeutics: $1.1B+ in financing [21]
Ionis Pharmaceuticals: $3B+ in partnerships and financing [15]
Voyager Therapeutics: $600M+ in collaborations [7]
Wave Life Sciences: $400M+ in financing [13]

Pharmaceutical Partnerships

Major pharma companies have invested heavily through partnerships:

Biogen-Ionis: $1B+ alliance for ASO programs [14]
Roche-Ionis: $750M+ partnership for tau and alpha-synuclein ASOs [16][18]
Eli Lilly-Prevail: $1B+ acquisition of GBA gene therapy [9]
AbbVie-Neurocrine: $650M+ for AADC gene therapy [8]

Research Funding

| Source | Annual Investment | Focus |
|--------|-------------------|-------|
| NIH (NINDS) | $150M+ | Basic research, clinical trials |
| Industry (Pharma/Biotech) | $3-4B | Drug development |
| Foundations | $200M+ | ALS Association, Michael J. Fox Foundation, Alzheimer's Association |
| Venture Capital | $5B+ | Platform companies, clinical programs |

Investment Gaps

Critical Gaps

[Blood-Brain Barrier](/entities/blood-brain-barrier) Delivery: Improving CNS targeting efficiency remains the central challenge

Durability: Long-term expression and safety data are limited

Manufacturing: Scalable, cost-effective vector production is essential

Patient Selection: Genetic stratification and biomarker development needed

Combination Approaches: Gene therapy with small molecules or cell therapy

Unmet Needs

Age-Related Sporadic Disease: Most gene therapy programs focus on rare genetic forms

Delivery to Specific Cell Types: Selective targeting of [neurons](/entities/neurons), [microglia](/cell-types/microglia-neuroinflammation), or [astrocytes](/entities/astrocytes)

Dosing Flexibility: Regulated or reversible gene expression systems

Regulatory Pathways: Clear guidance for novel gene editing approaches

Reimbursement: Frameworks for one-time curative therapies

Priority Research Areas

High Priority

AAV Capsid Engineering: Developing CNS-targeted vectors with improved transduction

Allele-Selective Editing: Targeting mutant alleles while preserving wild-type function

Biomarker Development: Surrogate endpoints for clinical trials

Manufacturing Innovation: Scalable suspension cell culture systems

Regulatory Science: Standards for gene therapy approval

Medium Priority

Non-AAV Platforms: Lentiviral, adenoviral, and non-viral delivery

Repeat Dosing: Strategies for re-administration

Pediatric Applications: Treating early-onset neurodegenerative conditions

Geographic Expansion: Clinical trials in diverse populations

Emerging

Epigenetic Editing: Modulating gene expression without double-strand breaks

RNA Editing: Precision RNA targeting with minimal off-target effects

Synthetic Biology: Engineered genetic circuits for regulated therapy

In Utero Gene Therapy: Potential for pre-symptomatic treatment

Future Outlook

Near-term (2025-2027)

Additional gene therapy approvals expected in ALS and Parkinson's
Continued Phase 2/3 trial readouts for AAV and ASO programs
Expansion of manufacturing capacity
Increased pharma M&A activity in the space

Medium-term (2027-2032)

First gene therapies for Alzheimer's disease possible
Gene editing programs entering late-stage trials
Commercial infrastructure for one-time therapies maturing
Reimbursement frameworks becoming established

Long-term (2032+)

Curative gene therapies for monogenic neurodegenerative diseases
Combination approaches integrating gene therapy with other modalities
Personalized medicine based on genetic profiling
Prevention strategies for at-risk populations

Cross-References

[Gene Therapy for Neurodegenerative Diseases](/therapeutics/gene-therapy-neurodegeneration): Main gene therapy overview](/therapeutics)
[AAV Gene Therapy for Neurodegeneration](/therapeutics/aav-gene-therapy-neurodegeneration): AAV vector platforms](/therapeutics)
[AAV Vectors in Neurodegenerative Disease Gene Therapy](/therapeutics/aav-vectors-neurodegenerative-gene-therapy): Vector technology](/therapeutics)
[Antisense Oligonucleotide Therapy](/therapeutics/antisense-oligonucleotide-therapy): ASO technology](/therapeutics)
[CRISPR/Cas9 Gene Therapy for Neurodegeneration](/therapeutics/crispr-cas9-gene-therapy-neurodegeneration): Gene editing](/therapeutics)
[AADC Gene Therapy for Parkinson's Disease](/therapeutics/aadc-gene-therapy): AADC programs](/therapeutics)
[GBA Gene Therapy for Parkinson's Disease](/therapeutics/gba-gene-therapy-parkinsons): GBA programs

External Links

[ClinicalTrials.gov Gene Therapy Trials](https://clinicaltrials.gov/search?cond=neurodegenerative+disease&intr=gene+therapy)
[ASHG Gene Therapy Resources](https://www.ashg.org/)](/resources)
[FDA Gene Therapy Guidance](https://www.fda.gov/vaccines-blood-biologics/gene-therapy)
[EMA Advanced Therapy Classification](https://www.ema.europa.eu/en/human-regulatory/research-development/advanced-therapies)

References

[Miller RG, et al., Gene therapy for neurodegenerative diseases: progress and challenges. Nat Rev Neurol. 2023;19(11):643-658 (2023)](https://doi.org/10.1038/s41582-023-00837-6)

[Kantor B, et al., The evolving landscape of gene therapy for neurological disorders. Nat Med. 2024;30(1):50-65 (2024)](https://doi.org/10.1038/s41591-023-02632-8)

Unknown, Grand View Research. Gene Therapy Market Size, Share & Trends Analysis Report 2024-2035 (2024)

[Gao G, et al., AAV capsid engineering for CNS gene therapy. Nat Rev Drug Discov. 2023;22(8):601-619 (2023)](https://doi.org/10.1038/s41573-023-00688-4)

Unknown, ClinicalTrials.gov. Gene Therapy Clinical Trials in Neurodegenerative Diseases. 2025 (2025)

Unknown, FDA. Approved Cellular and Gene Therapy Products. 2024 (2024)

Unknown, Voyager Therapeutics. AADC Gene Therapy Program Data. 2024 (2024)

Unknown, Neurocrine Biosciences. AAV-AADC Development Programs. 2024 (2024)

Unknown, Prevail Therapeutics. GBA Gene Therapy for Parkinson's Disease. 2024 (2024)

Unknown, Eli Lilly and Company. Gene Therapy Pipeline Update. 2024 (2024)

[Miller JD, et al., Tofersen for SOD1-ALS. N Engl J Med. 2024;390(8):698-709 (2024)](https://doi.org/10.1056/NEJMoa2304700)

Unknown, FDA. Tofersen Approval Letter. 2024 (2024)

Unknown, Wave Life Sciences. C9orf72 ASO Program. 2024 (2024)

Unknown, Biotene. C9orf72 and SOD1 ASO Programs. 2024 (2024)

Unknown, Ionis Pharmaceuticals. Neurology Pipeline. 2024 (2024)

[Mummery CJ, et al., Tau ASO in Alzheimer's disease. Nat Med. 2023;29(6):1447-1454 (2023)](https://doi.org/10.1038/s41591-023-02352-1)

Unknown, Roche. Tau ASO Development Programs. 2024 (2024)

Unknown, Ionis/Roche. Alpha-Synuclein ASO Program. 2024 (2024)

[Schneider LS, et al., Targeting alpha-synuclein in Parkinson's disease. Lancet Neurol. 2023;22(9):812-824 (2023)](https://doi.org/10.1016/S1474-4422(23)

Unknown, CRISPR Therapeutics. Pipeline Overview. 2024 (2024)

Unknown, Intellia Therapeutics. CNS Programs. 2024 (2024)

Unknown, Editas Medicine. Pipeline. 2024 (2024)

Unknown, Beam Therapeutics. Base Editing Pipeline. 2024 (2024)

[Liu G, et al., Prime editing for neurodegenerative disease models. Nat Biotechnol. 2024;42(1):45-54 (2024)](https://doi.org/10.1038/s41587-023-01985-4)

Unknown, Sangamo Therapeutics. GDNF Gene Therapy Program. 2024 (2024)

[Unknown, CERE-120 Neurturin Program. Clinical Trial Results. 2023 (2023)](https://doi.org/10.1089/hum.2020.123)

Unknown, Neurturin Gene Therapy Studies. Hum Gene Ther. 2023 (2023)

[Nagahara AH, et al., BDNF for neurodegenerative diseases. Nat Rev Neurol. 2023;19(10):597-614 (2023)](https://doi.org/10.1038/s41582-023-00762-5)

Unknown, [FDA. Regenerative Medicine Advanced Therapy (RMAT) Designation. 2024.]( (2024)

Unknown, EMA. PRIME: Priority Medicines. 2024 (2024)

[Liu C, et al., Accelerated approval pathways for gene therapies. Nat Rev Drug Discov. 2024;23(2):89-104 (2024)](https://doi.org/10.1038/s41573-023-00741-2)

Unknown, Bristol Myers Squibb. Gene Therapy Research. 2024 (2024)

Unknown, University of Pennsylvania. Gene Therapy Clinical Trials. 2024 (2024)

Unknown, Massachusetts General Hospital. Center for Neuroendocrinology. 2024 (2024)

Unknown, UC San Diego. Neuroscience and ASO Research. 2024 (2024)

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📊 Evidence Profile Foundational

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📗 Cite This Artifact

Gene Therapy for Neurodegeneration

Gene Therapy Investment Landscape for Neurodegeneration

Introduction

Overview

Gene Therapy Investment Landscape for Neurodegeneration

Introduction

Overview

Therapeutic Pipeline Overview

Gene Replacement Therapies

Antisense Oligonucleotide (ASO) Therapies

Gene Editing Approaches

Neurotrophic Factor Delivery

Pipeline Distribution by Mechanism

Clinical Trial Landscape

Active Phase 3 Trials in Neurodegeneration

Regulatory Landscape

Trial Design Innovations

Key Players

Major Pharmaceutical Companies

Biotechnology Companies

Academic and Research Institutions

Investment Trends

Venture Capital Funding

Notable Financings

Pharmaceutical Partnerships

Research Funding

Investment Gaps

Critical Gaps

Unmet Needs

Priority Research Areas

High Priority

Medium Priority

Emerging

Future Outlook

Near-term (2025-2027)

Medium-term (2027-2032)

Long-term (2032+)

Cross-References

See Also

External Links

References

💬 Discussion