Antiplatelet therapy guided by CYP2C19 point-of-care pharmacogenetics plus multidimensional treatment decisions

Author:

Voicu Victor12,Diehm Nicolas3,Moarof Igal4,Parejo Sarah5,Badiqué Florent5,Burden Andrea1,Niedrig David26,Béchir Markus7,Russmann Stefan1278ORCID

Affiliation:

1. Swiss Federal Institute of Technology Zurich (ETHZ), Switzerland

2. drugsafety.ch, 8700 Küsnacht ZH, Switzerland

3. Center for Vascular Medicine, 5000, Aarau, Switzerland

4. Cardiology Center Mittelland, 5001, Aarau, Switzerland

5. Medical Genetics Laboratory, Labor Risch, 3097, Berne-Liebefeld, Switzerland

6. Hospital Pharmacy, Clinic Hirslanden Zurich, 8032, Zurich, Switzerland

7. Center for Internal Medicine, Hirslanden Clinic Aarau, 5001 Aarau, Switzerland

8. University of Nicosia Medical School, 2408, Nicosia-Egkomi, Cyprus

Abstract

Aim: Implementation of CYP2C19 point-of-care (POC) pharmacogenetic (PGx) testing with personalized treatment recommendations. Methods: POC CYP2C19 genotyping plus expert evaluation of risk factors for ischemic and bleeding events. Results: 167 patients underwent PGx testing, 54 (32.3%) were CYP2C19 loss of function carriers, and POC versus standard PGx analysis results for *2 and *3 variants matched in 100%. Antiplatelet therapy was adjusted in 44 patients (26.3%), but always required consideration of patient-specific factors. Conclusion: CYP2C19 POC-PGx is reliable and offers clinically relevant advantages for immediate evidence-based adaptations of antiplatelet therapy, whereas in less acute cases conventional PGx testing can also have advantages. Antiplatelet therapy has become more complex, and implementation of PGx-based personalized antiplatelet therapy requires complementary expert knowledge.

Publisher

Future Medicine Ltd

Subject

Pharmacology,Genetics,Molecular Medicine

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