Metabolism of ticagrelor in patients with acute coronary syndromes

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作者
Piotr Adamski
Katarzyna Buszko
Joanna Sikora
Piotr Niezgoda
Malwina Barańska
Małgorzata Ostrowska
Przemysław Paciorek
Eliano P. Navarese
Diana A. Gorog
Jacek Kubica
机构
[1] Collegium Medicum,Department of Cardiology and Internal Medicine
[2] Nicolaus Copernicus University,Department of Theoretical Foundations of Biomedical Science and Medical Informatics, Collegium Medicum
[3] Nicolaus Copernicus University,Department of Pharmacology and Therapy, Collegium Medicum
[4] Nicolaus Copernicus University,Inova Heart and Vascular Institute
[5] Inova Center for Thrombosis Research and Drug Development,SIRIO MEDICINE research network, Inova Heart and Vascular Institute
[6] Inova Center for Thrombosis Research and Drug Development,National Heart & Lung Institute
[7] Imperial College,undefined
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摘要
Ticagrelor is a state-of-the-art antiplatelet agent used for the treatment of patients with acute coronary syndromes (ACS). Unlike remaining oral P2Y12 receptor inhibitors ticagrelor does not require metabolic activation to exert its antiplatelet action. Still, ticagrelor is extensively metabolized by hepatic CYP3A enzymes, and AR-C124910XX is its only active metabolite. A post hoc analysis of patient-level (n = 117) pharmacokinetic data pooled from two prospective studies was performed to identify clinical characteristics affecting the degree of AR-C124910XX formation during the first six hours after 180 mg ticagrelor loading dose in the setting of ACS. Both linear and multiple regression analyses indicated that ACS patients presenting with ST-elevation myocardial infarction or suffering from diabetes mellitus are more likely to have decreased rate of ticagrelor metabolism during the acute phase of ACS. Administration of morphine during ACS was found to negatively influence transformation of ticagrelor into AR-C124910XX when assessed with linear regression analysis, but not with multiple regression analysis. On the other hand, smoking appears to increase the degree of ticagrelor transformation in ACS patients. Mechanisms underlying our findings and their clinical significance warrant further research.
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