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Dopamine Metabolism Enzymes Beyond COMT
Dopamine Metabolism Enzymes Beyond COMT
<div class="infobox infobox-company">
<div class="infobox-header">Enzyme Target Pipeline</div>
<div class="infobox-row"><strong>Key Targets:</strong> AADC, DBH, MAO-A</div>
<div class="infobox-row"><strong>Stage:</strong> Preclinical to Approved</div>
<div class="infobox-row"><strong>Approach:</strong> Gene therapy, small molecules</div>
</div>
While COMT inhibitors are well-established in Parkinson's disease treatment, several other enzymes in the dopamine metabolic pathway represent therapeutic targets for companies developing next-generation therapies. The dopamine system regulates locomotion, reward-based motivation, performance monitoring, and endocrine functions, and dopamine itself is involved in conditions including Parkinson's disease, schizophrenia, and addiction [@key]. This page covers companies targeting aromatic L-amino acid decarboxylase (AADC), dopamine beta-hydroxylase (DBH), monoamine oxidase A (MAO-A), and other dopamine metabolic enzymes [@key].
Key Enzymes and Targets
AADC (Aromatic L-Amino Acid Decarboxylase)
AADC converts levodopa to dopamine, and gene therapy targeting this enzyme offers a disease-modifying approach for Parkinson's disease treatment [@key]. Several companies are pursuing AADC gene therapy programs at various stages of clinical development.
Dopamine Metabolism Enzymes Beyond COMT
<div class="infobox infobox-company">
<div class="infobox-header">Enzyme Target Pipeline</div>
<div class="infobox-row"><strong>Key Targets:</strong> AADC, DBH, MAO-A</div>
<div class="infobox-row"><strong>Stage:</strong> Preclinical to Approved</div>
<div class="infobox-row"><strong>Approach:</strong> Gene therapy, small molecules</div>
</div>
While COMT inhibitors are well-established in Parkinson's disease treatment, several other enzymes in the dopamine metabolic pathway represent therapeutic targets for companies developing next-generation therapies. The dopamine system regulates locomotion, reward-based motivation, performance monitoring, and endocrine functions, and dopamine itself is involved in conditions including Parkinson's disease, schizophrenia, and addiction [@key]. This page covers companies targeting aromatic L-amino acid decarboxylase (AADC), dopamine beta-hydroxylase (DBH), monoamine oxidase A (MAO-A), and other dopamine metabolic enzymes [@key].
Key Enzymes and Targets
AADC (Aromatic L-Amino Acid Decarboxylase)
AADC converts levodopa to dopamine, and gene therapy targeting this enzyme offers a disease-modifying approach for Parkinson's disease treatment [@key]. Several companies are pursuing AADC gene therapy programs at various stages of clinical development.
| Company | Program | Mechanism | Stage |
|---------|---------|-----------|-------|
| Voyager Therapeutics | VY-AADC | AAV-AADC gene therapy | Phase 1 |
| AbbVie | ABBV-951 (foslevodopa) | Prodrug delivery | Phase 3 |
| Cerevel | Tavaborole | AADC gene therapy | Phase 2 |
| Pasadena | AADC gene therapy | AAV delivery | Preclinical |
DBH (Dopamine Beta-Hydroxylase)
DBH converts dopamine to norepinephrine, and DBH inhibition represents a mechanism to increase dopamine levels by preventing its conversion to norepinephrine [@key]. Companies including Rarecyte and AstraZeneca are developing DBH inhibitors targeting norepinephrine modulation and cardiovascular/CNS applications, though these programs remain in early research and discovery stages.
| Company | Program | Focus | Stage |
|---------|---------|-------|-------|
| Rarecyte | DBH inhibitors | Norepinephrine modulation | Research |
| AstraZeneca | DBH programs | Cardiovascular/CNS | Discovery |
MAO-A (Monoamine Oxidase A)
MAO-A metabolizes dopamine in the brain, and selective MAO-A inhibition represents an alternative to MAO-B inhibitors currently used in clinical practice [@key]. Multiple companies are conducting research on MAO-A inhibitors in the research phase.
| Company | Program | Status |
|---------|---------|--------|
| Multiple | MAO-A inhibitors | Research phase |
Gene Therapy Approaches
AADC Gene Therapy
AADC gene therapy uses AAV vectors to deliver the AADC gene directly to the striatum, enabling neurons to produce AADC and convert levodopa to dopamine more efficiently [@key]. This approach represents a fundamental shift from symptomatic treatment toward potentially disease-modifying interventions.
Companies with AADC Programs
| Company | Product | Approach | Status |
|---------|---------|----------|--------|
| Voyager Therapeutics | VY-AADC | AAV2-AADC | Phase 1 |
| AbbVie | ABBV-951 | Gene therapy | Phase 3 |
| Cerevel | Tavaborole | AAV-AADC | Phase 2 |
Clinical Benefits
AADC gene therapy may reduce levodopa requirements while providing more stable dopamine synthesis throughout the day [@key]. This approach has the potential to slow disease progression by maintaining more physiological dopamine levels and may reduce motor fluctuations that plague patients on long-term levodopa therapy.
Small Molecule Approaches
DBH Inhibitors
DBH inhibition prevents conversion of dopamine to norepinephrine, which preserves dopamine for receptor activation and may enhance dopaminergic signaling without directly increasing dopamine levels [@key]. Various research compounds targeting DBH are in the discovery stage of development.
| Target | Company | Compound | Stage |
|--------|---------|----------|-------|
| DBH | Various | Research compounds | Discovery |
MAO-A Inhibitors
While MAO-B inhibitors are standard of care in Parkinson's disease, selective MAO-A inhibition is being explored as an alternative approach to dopaminergic enhancement [@key]. Development of MAO-A inhibitors remains in the preclinical and discovery stages.
| Target | Development Stage |
|--------|------------------|
| MAO-A | Preclinical/Discovery |
Comparison of Enzyme Targets
| Enzyme | Function | Inhibition Effect | Current Status |
|--------|----------|-------------------|----------------|
| AADC | Levodopa → Dopamine | Gene therapy approach | Phase 1-3 |
| DBH | Dopamine → Norepinephrine | Preserves dopamine | Discovery |
| MAO-A | Dopamine breakdown | Alternative to MAO-B | Research |
| MAO-B | Dopamine breakdown | Widely used (approved) | Commercial |
| COMT | Dopamine breakdown | Widely used (approved) | Commercial |
Related Mechanisms
The therapeutic targets discussed on this page interact with broader dopamine biology, including dopamine metabolism pathways, dopamine biosynthesis, levodopa pharmacokinetics, and Parkinson's disease gene therapy approaches [@key]. Understanding these related mechanisms provides context for how enzyme targeting fits into overall treatment strategies.
For additional information, see related pages on dopamine metabolism, dopamine biosynthesis pathway, levodopa pharmacokinetics, and Parkinson's disease gene therapy treatments.
Cross-References
For information on specific companies, see the PD pipeline companies overview, Voyager Therapeutics profile, Cerevel Therapeutics profile, AbbVie profile, and the mechanism index.
External Links
Relevant scientific literature can be found on PubMed for AADC and DBH research. Clinical trial information is available through ClinicalTrials.gov.
References
Pathway Diagram
The following diagram shows the key molecular relationships involving Dopamine Metabolism Enzymes Beyond COMT discovered through SciDEX knowledge graph analysis:
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