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Related Experiment Video

Updated: May 14, 2026

Analyzing Platelet Subpopulations by Multi-color Flow Cytometry
08:04

Analyzing Platelet Subpopulations by Multi-color Flow Cytometry

Published on: June 10, 2025

Clopidogrel, CYP2C19, and a Black Box.

Neville F Ford1, Dirk Taubert

  • 1Woodfield Clinical Consulting LLC, Green Valley, AZ 85622, USA. neville@woodfieldclinical.com

Journal of Clinical Pharmacology
|February 6, 2013
PubMed
Summary
This summary is machine-generated.

Clopidogrel is primarily metabolized by CYP3A, not CYP2C19. This finding, supported by new in vitro data, explains why proton pump inhibitors do not increase cardiovascular events when used with clopidogrel.

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Area of Science:

  • Pharmacology
  • Drug Metabolism
  • Cardiovascular Medicine

Background:

  • Clopidogrel metabolism was presumed to be primarily via CYP2C19.
  • This led to concerns about drug interactions with CYP2C19 inhibitors like proton pump inhibitors (PPIs).
  • A FDA "Black Box" warning was issued in 2010 based on early in vitro and ex vivo studies.

Purpose of the Study:

  • To re-evaluate the primary metabolic pathway of clopidogrel.
  • To reconcile in vitro findings with clinical observations regarding clopidogrel and PPI co-administration.
  • To investigate the discrepancy between presumed CYP2C19 metabolism and clinical outcomes.

Main Methods:

  • Revisiting in vitro drug metabolism studies using "Supersomes".
  • Conducting new in vitro metabolism studies using hepatosomes, which better reflect native cytochrome P-450 enzyme expression.
  • Analyzing data from prospective clinical studies (e.g., COGENT) and meta-analyses.

Main Results:

  • In vitro studies using hepatosomes confirmed clopidogrel is primarily a CYP3A substrate.
  • This finding aligns with clinical data showing no increased risk of major adverse cardiovascular events (MACE) with concomitant clopidogrel and PPI use.
  • The absence of a significant interaction contradicts the initial presumption of CYP2C19 involvement.

Conclusions:

  • Clopidogrel's primary metabolism is via CYP3A, not CYP2C19.
  • The lack of interaction between clopidogrel and PPIs is explained by clopidogrel's actual metabolic pathway.
  • Further research may explore the role of CYP2C19 in specific patient populations with reduced function alleles.