Critical Pharmacodynamic Warning
metoclopramide weakly inhibits the 2D6 metabolic pathway.
When patients take metoclopramide concurrently with drugs metabolized by 2D6, the risk of adverse effects may significantly increase. This interaction affects drug clearance and systemic exposure, potentially leading to toxicity or reduced therapeutic efficacy.
Clinical Impact: As a weak inhibitor, metoclopramide can alter the metabolism of substrate drugs, requiring careful monitoring and potential dose adjustments.
Clinical Overview for metoclopramide
This page outlines known interaction pathways involving metoclopramide, focusing primarily on its profile as a Weak inhibitor affecting the 2D6 pathway.
Enzyme Interaction Profile
metoclopramide demonstrates weak inhibitor potency against 2D6. This level of inhibition causes ≥1.25-fold but <2-fold increase in AUC of substrate drugs.
Inhibitor
A substance that slows down or prevents an enzyme from metabolizing a drug. Inhibitors can lead to increased drug concentrations in the body, potentially causing toxicity or enhanced therapeutic effects.
Clinical Example: metoclopramide weakly inhibits 2D6Inducer
A substance that speeds up enzyme activity, causing drugs to be cleared from the body faster. Inducers can reduce drug effectiveness by lowering concentrations below therapeutic levels.
Interaction Details
| Drug Name | metoclopramide |
| Affected Enzyme | 2D6 |
| Inhibitor Strength | Weak inhibitor Low Severity |
| Inducers | No inducers listed |
| Inhibitors | citalopram |
Clinical Recommendations
Generally safe for co-administration. Routine monitoring recommended.
- Therapeutic drug levels
- Adverse effect monitoring
- Clinical response assessment
- Consider dose reduction
- Evaluate alternative therapies
- Adjust based on response
Quick Facts
2291
2D6
Enzyme Inhibition
Low Severity
Clinical Significance
Minor clinical significance. Routine monitoring sufficient.
Information Sources
- FDA Drug Interaction Database
- Clinical Pharmacology Guidelines
- Pharmaceutical Labeling Information
- Published Clinical Studies
Last updated: June 15, 2026